Biological Age: Difference between revisions
Line 640: | Line 640: | ||
{| class="wikitable" | {| class="wikitable" | ||
! System | ! System | ||
! | |||
! MLR | ! MLR | ||
! PCA | ! PCA | ||
Line 646: | Line 647: | ||
|- | |- | ||
| colspan="1" rowspan="17" |Cardiovascular system | | colspan="1" rowspan="17" |Cardiovascular system | ||
| | |||
| SBP{{pmid|23213031}}{{pmid|5841151}}{{pmid|3226152}}{{pmid|950448}}{{pmid|6667707}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}}{{pmid|30899733}} | | SBP{{pmid|23213031}}{{pmid|5841151}}{{pmid|3226152}}{{pmid|950448}}{{pmid|6667707}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}}{{pmid|30899733}} | ||
| SBP{{pmid|23213031}}{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}}{{pmid|12672981}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}}{{pmid|22433233}}{{pmid|28110151}}{{pmid|30899733}} | | SBP{{pmid|23213031}}{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}}{{pmid|12672981}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}}{{pmid|22433233}}{{pmid|28110151}}{{pmid|30899733}} | ||
Line 651: | Line 653: | ||
| | | | ||
|- | |- | ||
| | |||
| DBP{{pmid|17889950}}{{pmid|23642770}}{{pmid|31179487}} | | DBP{{pmid|17889950}}{{pmid|23642770}}{{pmid|31179487}} | ||
| DBP{{pmid|31179487}} | | DBP{{pmid|31179487}} | ||
Line 656: | Line 659: | ||
| | | | ||
|- | |- | ||
| | |||
| Pulse pressure{{pmid|23642770}} | | Pulse pressure{{pmid|23642770}} | ||
| Pulse pressure{{pmid|29188884}}{{pmid|24522464}}{{pmid|19940465}} | | Pulse pressure{{pmid|29188884}}{{pmid|24522464}}{{pmid|19940465}} | ||
Line 661: | Line 665: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Mean arterial pressure{{pmid|28203066}} | | Mean arterial pressure{{pmid|28203066}} | ||
Line 666: | Line 671: | ||
| | | | ||
|- | |- | ||
| | |||
| Pulse{{pmid|3226152}} | | Pulse{{pmid|3226152}} | ||
| Pulse{{pmid|3226152}}{{pmid|2737197}} | | Pulse{{pmid|3226152}}{{pmid|2737197}} | ||
Line 671: | Line 677: | ||
| | | | ||
|- | |- | ||
| | |||
| Pulse wave velocity{{pmid|6667707}} | | Pulse wave velocity{{pmid|6667707}} | ||
| | | | ||
Line 676: | Line 683: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Heart rate{{pmid|2282902}} | | Heart rate{{pmid|2282902}} | ||
Line 681: | Line 689: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Intima-media thickness{{pmid|24659482}}{{pmid|19940465}} | | Intima-media thickness{{pmid|24659482}}{{pmid|19940465}} | ||
Line 686: | Line 695: | ||
| | | | ||
|- | |- | ||
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| | | | ||
| Minimum intima-media | | Minimum intima-media | ||
Line 692: | Line 702: | ||
| | | | ||
|- | |- | ||
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| | | | ||
| End diastolic velocity{{pmid|19940465}} | | End diastolic velocity{{pmid|19940465}} | ||
Line 697: | Line 708: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| mitral valve E/A peak{{pmid|29188884}}{{pmid|19940465}} | | mitral valve E/A peak{{pmid|29188884}}{{pmid|19940465}} | ||
Line 702: | Line 714: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| MVEL{{pmid|19940465}}, MVES{{pmid|24522464}}, MVEA{{pmid|24659482}} | | MVEL{{pmid|19940465}}, MVES{{pmid|24522464}}, MVEA{{pmid|24659482}} | ||
Line 707: | Line 720: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Atherosclerosis index{{pmid|2737197}}{{pmid|2282902}} | | Atherosclerosis index{{pmid|2737197}}{{pmid|2282902}} | ||
Line 712: | Line 726: | ||
| | | | ||
|- | |- | ||
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| | | | ||
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Line 717: | Line 732: | ||
| NT-proBNP{{pmid|34453631}} | | NT-proBNP{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 722: | Line 738: | ||
| Cardiac troponin I{{pmid|34453631}} | | Cardiac troponin I{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Creatine phosphokinase{{pmid|23642770}} | | Creatine phosphokinase{{pmid|23642770}} | ||
| | | | ||
Line 727: | Line 744: | ||
| | | | ||
|- | |- | ||
| | |||
| Homocysteine{{pmid|23642770}} | | Homocysteine{{pmid|23642770}} | ||
| | | | ||
Line 734: | Line 752: | ||
| colspan="1" rowspan="6" |Respiratory | | colspan="1" rowspan="6" |Respiratory | ||
system | system | ||
| | |||
| FVC{{pmid|3226152}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|20005245}} | | FVC{{pmid|3226152}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|20005245}} | ||
| FVC{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}} | | FVC{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}} | ||
Line 739: | Line 758: | ||
| | | | ||
|- | |- | ||
| | |||
| FEV1{{pmid|23213031}}{{pmid|950448}}{{pmid|7162237}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}}{{pmid|30899733}}{{pmid|31179487}} | | FEV1{{pmid|23213031}}{{pmid|950448}}{{pmid|7162237}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}}{{pmid|30899733}}{{pmid|31179487}} | ||
| FEV1{{pmid|23213031}}{{pmid|12634284}}{{pmid|12672981}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}}{{pmid|22433233}}{{pmid|28110151}}{{pmid|30899733}}{{pmid|31179487}} | | FEV1{{pmid|23213031}}{{pmid|12634284}}{{pmid|12672981}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}}{{pmid|22433233}}{{pmid|28110151}}{{pmid|30899733}}{{pmid|31179487}} | ||
Line 744: | Line 764: | ||
| | | | ||
|- | |- | ||
| | |||
| Vital capacity{{pmid|5841151}}{{pmid|6667707}} | | Vital capacity{{pmid|5841151}}{{pmid|6667707}} | ||
| | | | ||
Line 749: | Line 770: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Maximal midexpiratory | | Maximal midexpiratory | ||
Line 755: | Line 777: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| VO2 max{{pmid|18597867}}{{pmid|22433233}} | | VO2 max{{pmid|18597867}}{{pmid|22433233}} | ||
Line 760: | Line 783: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 766: | Line 790: | ||
|- | |- | ||
| colspan="1" rowspan="9" |Nervous system | | colspan="1" rowspan="9" |Nervous system | ||
| | |||
| MMSE{{pmid|31179487}} | | MMSE{{pmid|31179487}} | ||
| MMSE{{pmid|31179487}} | | MMSE{{pmid|31179487}} | ||
Line 771: | Line 796: | ||
| | | | ||
|- | |- | ||
| | |||
| Digital symbol test{{pmid|6667707}} | | Digital symbol test{{pmid|6667707}} | ||
| Digital symbol test{{pmid|24659482}} | | Digital symbol test{{pmid|24659482}} | ||
Line 776: | Line 802: | ||
| | | | ||
|- | |- | ||
| | |||
| Numeric memory{{pmid|20005245}} | | Numeric memory{{pmid|20005245}} | ||
| | | | ||
Line 781: | Line 808: | ||
| | | | ||
|- | |- | ||
| | |||
| Associated memory{{pmid|20005245}} | | Associated memory{{pmid|20005245}} | ||
| | | | ||
Line 786: | Line 814: | ||
| | | | ||
|- | |- | ||
| | |||
| Topological memory{{pmid|20005245}} | | Topological memory{{pmid|20005245}} | ||
| | | | ||
Line 791: | Line 820: | ||
| | | | ||
|- | |- | ||
| | |||
| Short-time memory{{pmid|6610563}} | | Short-time memory{{pmid|6610563}} | ||
| | | | ||
Line 796: | Line 826: | ||
| | | | ||
|- | |- | ||
| | |||
| Concentration{{pmid|20005245}} | | Concentration{{pmid|20005245}} | ||
| | | | ||
Line 801: | Line 832: | ||
| | | | ||
|- | |- | ||
| | |||
| Intellectuality -mental defect{{pmid|6667707}} | | Intellectuality -mental defect{{pmid|6667707}} | ||
| | | | ||
Line 806: | Line 838: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Trail making test{{pmid|29188884}}{{pmid|24522464}} | | Trail making test{{pmid|29188884}}{{pmid|24522464}} | ||
Line 812: | Line 845: | ||
|- | |- | ||
| colspan="1" rowspan="15" |Endocrine metabolic system | | colspan="1" rowspan="15" |Endocrine metabolic system | ||
| | |||
| Glucose{{pmid|17889950}}{{pmid|23642770}} | | Glucose{{pmid|17889950}}{{pmid|23642770}} | ||
| Glucose{{pmid|8803500}}{{pmid|12672981}}{{pmid|28203066}} | | Glucose{{pmid|8803500}}{{pmid|12672981}}{{pmid|28203066}} | ||
Line 817: | Line 851: | ||
| Glucose{{pmid|27191382}}{{pmid|29340580}}{{pmid|30644411}}{{pmid|34453631}} | | Glucose{{pmid|27191382}}{{pmid|29340580}}{{pmid|30644411}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| HBA1C{{pmid|23213031}}{{pmid|23642770}} | | HBA1C{{pmid|23213031}}{{pmid|23642770}} | ||
| HBA1C{{pmid|23213031}}{{pmid|18597867}} | | HBA1C{{pmid|23213031}}{{pmid|18597867}} | ||
Line 822: | Line 857: | ||
| HBA1C{{pmid|30644411}} | | HBA1C{{pmid|30644411}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 827: | Line 863: | ||
| C-peptide{{pmid|34453631}} | | C-peptide{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 832: | Line 869: | ||
| Insulin{{pmid|34453631}} | | Insulin{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Triglyceride{{pmid|950448}}{{pmid|17889950}}{{pmid|23642770}} | | Triglyceride{{pmid|950448}}{{pmid|17889950}}{{pmid|23642770}} | ||
| Triglyceride{{pmid|2282902}}{{pmid|28203066}} | | Triglyceride{{pmid|2282902}}{{pmid|28203066}} | ||
Line 837: | Line 875: | ||
| Triglyceride{{pmid|29340580}}{{pmid|34453631}} | | Triglyceride{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| TC{{pmid|23213031}}{{pmid|5841151}}{{pmid|3226152}}{{pmid|950448}}{{pmid|7162237}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}} | | TC{{pmid|23213031}}{{pmid|5841151}}{{pmid|3226152}}{{pmid|950448}}{{pmid|7162237}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}} | ||
| TC{{pmid|23213031}}{{pmid|3226152}}{{pmid|8803500}}{{pmid|28110151}} | | TC{{pmid|23213031}}{{pmid|3226152}}{{pmid|8803500}}{{pmid|28110151}} | ||
Line 842: | Line 881: | ||
| TC{{pmid|27191382}}{{pmid|29340580}} | | TC{{pmid|27191382}}{{pmid|29340580}} | ||
|- | |- | ||
| | |||
| HDL{{pmid|17889950}}, LDL{{pmid|23642770}} | | HDL{{pmid|17889950}}, LDL{{pmid|23642770}} | ||
| HDL{{pmid|28203066}}, LDL{{pmid|18597867}} | | HDL{{pmid|28203066}}, LDL{{pmid|18597867}} | ||
Line 847: | Line 887: | ||
| HDL{{pmid|29340580}}{{pmid|34453631}},LDL{{pmid|29340580}}{{pmid|34453631}} | | HDL{{pmid|29340580}}{{pmid|34453631}},LDL{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 852: | Line 893: | ||
| Apolipoprotein A1 and B{{pmid|34453631}} | | Apolipoprotein A1 and B{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| TSH{{pmid|17889950}} | | TSH{{pmid|17889950}} | ||
| | | | ||
Line 857: | Line 899: | ||
| | | | ||
|- | |- | ||
| | |||
| Testosterone{{pmid|17889950}} | | Testosterone{{pmid|17889950}} | ||
| | | | ||
Line 862: | Line 905: | ||
| Testosterone{{pmid|34453631}} | | Testosterone{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Vitamin D{{pmid|30899733}} | | Vitamin D{{pmid|30899733}} | ||
| Vitamin D{{pmid|30899733}} | | Vitamin D{{pmid|30899733}} | ||
Line 867: | Line 911: | ||
| Vitamin D{{pmid|34453631}} | | Vitamin D{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 872: | Line 917: | ||
| Calcium{{pmid|29340580}} | | Calcium{{pmid|29340580}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 877: | Line 923: | ||
| Potassium{{pmid|29340580}} | | Potassium{{pmid|29340580}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 882: | Line 929: | ||
| Sodium{{pmid|29340580}} | | Sodium{{pmid|29340580}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 888: | Line 936: | ||
|- | |- | ||
| colspan="1" rowspan="8" |Urinary system | | colspan="1" rowspan="8" |Urinary system | ||
| | |||
| Urea{{pmid|23213031}}{{pmid|3226152}}{{pmid|950448}}{{pmid|23642770}}{{pmid|28110151}} | | Urea{{pmid|23213031}}{{pmid|3226152}}{{pmid|950448}}{{pmid|23642770}}{{pmid|28110151}} | ||
| Urea{{pmid|23213031}}{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}}{{pmid|28110151}} | | Urea{{pmid|23213031}}{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}}{{pmid|28110151}} | ||
Line 893: | Line 942: | ||
| Urea{{pmid|27191382}}{{pmid|29340580}}{{pmid|30644411}} | | Urea{{pmid|27191382}}{{pmid|29340580}}{{pmid|30644411}} | ||
|- | |- | ||
| | |||
| Creatinine{{pmid|23213031}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}}{{pmid|30899733}} | | Creatinine{{pmid|23213031}}{{pmid|17889950}}{{pmid|23642770}}{{pmid|28110151}}{{pmid|30899733}} | ||
| Creatinine{{pmid|28110151}}{{pmid|30899733}} | | Creatinine{{pmid|28110151}}{{pmid|30899733}} | ||
Line 898: | Line 948: | ||
| Creatinine{{pmid|29340580}}{{pmid|34453631}} | | Creatinine{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| eGFR{{pmid|31179487}} | | eGFR{{pmid|31179487}} | ||
| eGFR{{pmid|31179487}} | | eGFR{{pmid|31179487}} | ||
Line 903: | Line 954: | ||
| | | | ||
|- | |- | ||
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| | | | ||
| | | | ||
Line 908: | Line 960: | ||
| Uric acid{{pmid|34453631}} | | Uric acid{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| Cystatin C{{pmid|29188884}}{{pmid|24659482}}{{pmid|24522464}}{{pmid|19940465}} | | Cystatin C{{pmid|29188884}}{{pmid|24659482}}{{pmid|24522464}}{{pmid|19940465}} | ||
Line 913: | Line 966: | ||
| Cystatin C{{pmid|34453631}} | | Cystatin C{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Creatinine clearance{{pmid|23642770}} | | Creatinine clearance{{pmid|23642770}} | ||
| | | | ||
Line 918: | Line 972: | ||
| | | | ||
|- | |- | ||
| | |||
| Urine specific gravity{{pmid|23642770}} | | Urine specific gravity{{pmid|23642770}} | ||
| | | | ||
Line 923: | Line 978: | ||
| | | | ||
|- | |- | ||
| | |||
| Urine pH{{pmid|23642770}} | | Urine pH{{pmid|23642770}} | ||
| | | | ||
Line 929: | Line 985: | ||
|- | |- | ||
| colspan="1" rowspan="12" |Digestive system | | colspan="1" rowspan="12" |Digestive system | ||
| | |||
| ALT{{pmid|23642770}} | | ALT{{pmid|23642770}} | ||
| ALT{{pmid|8803500}} | | ALT{{pmid|8803500}} | ||
Line 934: | Line 991: | ||
| ALT{{pmid|34453631}} | | ALT{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| AST{{pmid|3226152}}{{pmid|23642770}}{{pmid|28110151}} | | AST{{pmid|3226152}}{{pmid|23642770}}{{pmid|28110151}} | ||
| AST{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|28110151}} | | AST{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|28110151}} | ||
Line 939: | Line 997: | ||
| AST{{pmid|34453631}} | | AST{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| ALP{{pmid|23213031}}{{pmid|950448}}{{pmid|23642770}} | | ALP{{pmid|23213031}}{{pmid|950448}}{{pmid|23642770}} | ||
| ALP{{pmid|23213031}} | | ALP{{pmid|23213031}} | ||
Line 944: | Line 1,003: | ||
| ALP{{pmid|27191382}} | | ALP{{pmid|27191382}} | ||
|- | |- | ||
| | |||
| Total protein{{pmid|23642770}} | | Total protein{{pmid|23642770}} | ||
| | | | ||
Line 949: | Line 1,009: | ||
| Total protein{{pmid|29340580}} | | Total protein{{pmid|29340580}} | ||
|- | |- | ||
| | |||
| Albumin{{pmid|23213031}}{{pmid|3226152}}{{pmid|23642770}} | | Albumin{{pmid|23213031}}{{pmid|3226152}}{{pmid|23642770}} | ||
| Albumin{{pmid|23213031}}{{pmid|3226152}}{{pmid|12634284}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}} | | Albumin{{pmid|23213031}}{{pmid|3226152}}{{pmid|12634284}}{{pmid|17921421}}{{pmid|18840798}}{{pmid|18597867}} | ||
Line 954: | Line 1,015: | ||
| Albumin{{pmid|27191382}}{{pmid|29340580}}{{pmid|34453631}} | | Albumin{{pmid|27191382}}{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| A/G{{pmid|3226152}}{{pmid|23642770}} | | A/G{{pmid|3226152}}{{pmid|23642770}} | ||
| A/G{{pmid|3226152}}{{pmid|12634284}}{{pmid|12672981}} | | A/G{{pmid|3226152}}{{pmid|12634284}}{{pmid|12672981}} | ||
Line 959: | Line 1,021: | ||
| | | | ||
|- | |- | ||
| | |||
| Total bilirubin{{pmid|23642770}} | | Total bilirubin{{pmid|23642770}} | ||
| | | | ||
Line 964: | Line 1,027: | ||
| Total bilirubin{{pmid|29340580}} | | Total bilirubin{{pmid|29340580}} | ||
|- | |- | ||
| | |||
| Direct bilirubin{{pmid|23642770}} | | Direct bilirubin{{pmid|23642770}} | ||
| | | | ||
Line 969: | Line 1,033: | ||
| | | | ||
|- | |- | ||
| | |||
| Amylase{{pmid|23642770}} | | Amylase{{pmid|23642770}} | ||
| | | | ||
Line 974: | Line 1,039: | ||
| | | | ||
|- | |- | ||
| | |||
| Lactate dehydrogenase{{pmid|7162237}}{{pmid|23642770}} | | Lactate dehydrogenase{{pmid|7162237}}{{pmid|23642770}} | ||
| Lactate dehydrogenase{{pmid|2282902}}{{pmid|8803500}} | | Lactate dehydrogenase{{pmid|2282902}}{{pmid|8803500}} | ||
Line 979: | Line 1,045: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 984: | Line 1,051: | ||
| Alpha 2 globulin{{pmid|27191382}} | | Alpha 2 globulin{{pmid|27191382}} | ||
|- | |- | ||
| | |||
| Gamma glutamyl | | Gamma glutamyl | ||
transpeptidase{{pmid|23642770}} | transpeptidase{{pmid|23642770}} | ||
Line 991: | Line 1,059: | ||
|- | |- | ||
| colspan="1" rowspan="21" |Hematologic System | | colspan="1" rowspan="21" |Hematologic System | ||
| | |||
| Red blood cell{{pmid|30899733}} | | Red blood cell{{pmid|30899733}} | ||
| Red blood cell{{pmid|12634284}}{{pmid|18840798}}{{pmid|30899733}} | | Red blood cell{{pmid|12634284}}{{pmid|18840798}}{{pmid|30899733}} | ||
Line 996: | Line 1,065: | ||
| Red blood cell{{pmid|27191382}}{{pmid|29340580}}{{pmid|34453631}} | | Red blood cell{{pmid|27191382}}{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,003: | Line 1,073: | ||
distribution width{{pmid|27191382}}{{pmid|34453631}} | distribution width{{pmid|27191382}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| Hematocrit{{pmid|12634284}}{{pmid|17921421}} | | Hematocrit{{pmid|12634284}}{{pmid|17921421}} | ||
Line 1,008: | Line 1,079: | ||
| Hematocrit{{pmid|27191382}}{{pmid|29340580}} | | Hematocrit{{pmid|27191382}}{{pmid|29340580}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,015: | Line 1,087: | ||
volume{{pmid|29340580}}{{pmid|34453631}} | volume{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| Mean corpuscular | | Mean corpuscular | ||
Line 1,021: | Line 1,094: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,026: | Line 1,100: | ||
| Mean corpuscular hemoglobin concentration{{pmid|29340580}}{{pmid|34453631}} | | Mean corpuscular hemoglobin concentration{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Hemoglobin{{pmid|3226152}}{{pmid|31179487}} | | Hemoglobin{{pmid|3226152}}{{pmid|31179487}} | ||
| Hemoglobin{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}}{{pmid|31179487}} | | Hemoglobin{{pmid|3226152}}{{pmid|2737197}}{{pmid|2282902}}{{pmid|8803500}}{{pmid|12634284}}{{pmid|31179487}} | ||
Line 1,031: | Line 1,106: | ||
| Hemoglobin{{pmid|29340580}}{{pmid|34453631}} | | Hemoglobin{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,036: | Line 1,112: | ||
| White blood cell{{pmid|34453631}} | | White blood cell{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,041: | Line 1,118: | ||
| Granulocytes{{pmid|34453631}} | | Granulocytes{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,046: | Line 1,124: | ||
| Neutrophils{{pmid|34453631}} | | Neutrophils{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,051: | Line 1,130: | ||
| Basophils{{pmid|34453631}}, Eosinophils{{pmid|34453631}} | | Basophils{{pmid|34453631}}, Eosinophils{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,056: | Line 1,136: | ||
| Lymphocytes{{pmid|27191382}}{{pmid|34453631}} | | Lymphocytes{{pmid|27191382}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Monocytes{{pmid|31179487}} | | Monocytes{{pmid|31179487}} | ||
| Monocytes{{pmid|31179487}} | | Monocytes{{pmid|31179487}} | ||
Line 1,061: | Line 1,142: | ||
| Monocytes{{pmid|34453631}} | | Monocytes{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,066: | Line 1,148: | ||
| Platelet{{pmid|29340580}}{{pmid|34453631}} | | Platelet{{pmid|29340580}}{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,071: | Line 1,154: | ||
| Mean platelet volume{{pmid|34453631}} | | Mean platelet volume{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,076: | Line 1,160: | ||
| Platelet distribution width{{pmid|34453631}} | | Platelet distribution width{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Erythrocyte | | Erythrocyte | ||
| Erythrocyte | | Erythrocyte | ||
Line 1,081: | Line 1,166: | ||
| | | | ||
|- | |- | ||
| | |||
| sedimentation rat{{pmid|950448}}{{pmid|17889950}} | | sedimentation rat{{pmid|950448}}{{pmid|17889950}} | ||
| sedimentation rat{{pmid|18597867}} | | sedimentation rat{{pmid|18597867}} | ||
Line 1,086: | Line 1,172: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| D-dimer{{pmid|24659482}} | | D-dimer{{pmid|24659482}} | ||
Line 1,092: | Line 1,179: | ||
| D-dimer{{pmid|34453631}} | | D-dimer{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Ferritin{{pmid|28110151}} | | Ferritin{{pmid|28110151}} | ||
| Ferritin{{pmid|28110151}} | | Ferritin{{pmid|28110151}} | ||
Line 1,097: | Line 1,185: | ||
| Ferritin{{pmid|30644411}} | | Ferritin{{pmid|30644411}} | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,103: | Line 1,192: | ||
|- | |- | ||
| colspan="1" rowspan="6" |Sensory system | | colspan="1" rowspan="6" |Sensory system | ||
| | |||
| Visual accommodation{{pmid|6667707}}{{pmid|20005245}} | | Visual accommodation{{pmid|6667707}}{{pmid|20005245}} | ||
| | | | ||
Line 1,108: | Line 1,198: | ||
| | | | ||
|- | |- | ||
| | |||
| Visual reaction time{{pmid|20005245}} | | Visual reaction time{{pmid|20005245}} | ||
| | | | ||
Line 1,113: | Line 1,204: | ||
| | | | ||
|- | |- | ||
| | |||
| Visual acuity{{pmid|5841151}}{{pmid|3226152}} | | Visual acuity{{pmid|5841151}}{{pmid|3226152}} | ||
| Visual acuity{{pmid|3226152}} | | Visual acuity{{pmid|3226152}} | ||
Line 1,118: | Line 1,210: | ||
| | | | ||
|- | |- | ||
| | |||
| Hearing{{pmid|5841151}}{{pmid|7162237}}{{pmid|6667707}}{{pmid|20005245}} | | Hearing{{pmid|5841151}}{{pmid|7162237}}{{pmid|6667707}}{{pmid|20005245}} | ||
| Hearing{{pmid|18597867}} | | Hearing{{pmid|18597867}} | ||
Line 1,123: | Line 1,216: | ||
| | | | ||
|- | |- | ||
| | |||
| Vibrotactile{{pmid|5841151}}{{pmid|6610563}}{{pmid|20005245}} | | Vibrotactile{{pmid|5841151}}{{pmid|6610563}}{{pmid|20005245}} | ||
| | | | ||
Line 1,128: | Line 1,222: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,134: | Line 1,229: | ||
|- | |- | ||
| colspan="1" rowspan="4" |Inflammatory index | | colspan="1" rowspan="4" |Inflammatory index | ||
| | |||
| CRP{{pmid|23213031}} | | CRP{{pmid|23213031}} | ||
| CRP{{pmid|23213031}} | | CRP{{pmid|23213031}} | ||
Line 1,139: | Line 1,235: | ||
| CRP{{pmid|34453631}} | | CRP{{pmid|34453631}} | ||
|- | |- | ||
| | |||
| Cytomegalovirus optical density{{pmid|23213031}} | | Cytomegalovirus optical density{{pmid|23213031}} | ||
| Cytomegalovirus | | Cytomegalovirus | ||
Line 1,146: | Line 1,243: | ||
| | | | ||
|- | |- | ||
| | |||
| colspan="1" rowspan="2" | | | colspan="1" rowspan="2" | | ||
| colspan="1" rowspan="2" | | | colspan="1" rowspan="2" | | ||
Line 1,151: | Line 1,249: | ||
| colspan="1" rowspan="2" | | | colspan="1" rowspan="2" | | ||
|- | |- | ||
| | |||
| P-selectin{{pmid|28977464}} | | P-selectin{{pmid|28977464}} | ||
|- | |- | ||
| colspan="1" rowspan="5" |Motion index | | colspan="1" rowspan="5" |Motion index | ||
| | |||
| Grip strength{{pmid|5841151}}{{pmid|6610563}}{{pmid|31179487}}{{pmid|20005245}} | | Grip strength{{pmid|5841151}}{{pmid|6610563}}{{pmid|31179487}}{{pmid|20005245}} | ||
| Grip strength{{pmid|22433233}}{{pmid|31179487}} | | Grip strength{{pmid|22433233}}{{pmid|31179487}} | ||
Line 1,159: | Line 1,259: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Vertical jump{{pmid|22433233}} | | Vertical jump{{pmid|22433233}} | ||
Line 1,164: | Line 1,265: | ||
| | | | ||
|- | |- | ||
| | |||
| Timed up and go test{{pmid|31179487}} | | Timed up and go test{{pmid|31179487}} | ||
| Timed up and go test{{pmid|31179487}} | | Timed up and go test{{pmid|31179487}} | ||
Line 1,169: | Line 1,271: | ||
| | | | ||
|- | |- | ||
| | |||
| Chair rise time{{pmid|31179487}} | | Chair rise time{{pmid|31179487}} | ||
| Chair rise time{{pmid|31179487}} | | Chair rise time{{pmid|31179487}} | ||
Line 1,174: | Line 1,277: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| | | | ||
Line 1,180: | Line 1,284: | ||
|- | |- | ||
| colspan="1" rowspan="9" |Body morphology index | | colspan="1" rowspan="9" |Body morphology index | ||
| | |||
| WC{{pmid|23642770}}{{pmid|28110151}} | | WC{{pmid|23642770}}{{pmid|28110151}} | ||
| WC{{pmid|18597867}}{{pmid|22433233}}{{pmid|28110151}}{{pmid|28203066}} | | WC{{pmid|18597867}}{{pmid|22433233}}{{pmid|28110151}}{{pmid|28203066}} | ||
Line 1,185: | Line 1,290: | ||
| | | | ||
|- | |- | ||
| | |||
| Waist-to-hip ratio{{pmid|17889950}}{{pmid|23642770}} | | Waist-to-hip ratio{{pmid|17889950}}{{pmid|23642770}} | ||
| | | | ||
Line 1,190: | Line 1,296: | ||
| | | | ||
|- | |- | ||
| | |||
| Waist-to-height ratio{{pmid|30899733}} | | Waist-to-height ratio{{pmid|30899733}} | ||
| Waist-to-height ratio{{pmid|30899733}} | | Waist-to-height ratio{{pmid|30899733}} | ||
Line 1,195: | Line 1,302: | ||
| | | | ||
|- | |- | ||
| | |||
| Body mass index{{pmid|17889950}}{{pmid|23642770}} | | Body mass index{{pmid|17889950}}{{pmid|23642770}} | ||
| | | | ||
Line 1,200: | Line 1,308: | ||
| | | | ||
|- | |- | ||
| | |||
| Weight{{pmid|6667707}} | | Weight{{pmid|6667707}} | ||
| | | | ||
Line 1,205: | Line 1,314: | ||
| | | | ||
|- | |- | ||
| | |||
| Height{{pmid|31179487}} | | Height{{pmid|31179487}} | ||
| Height{{pmid|31179487}} | | Height{{pmid|31179487}} | ||
Line 1,210: | Line 1,320: | ||
| | | | ||
|- | |- | ||
| | |||
| Body fat{{pmid|17889950}}{{pmid|23642770}} | | Body fat{{pmid|17889950}}{{pmid|23642770}} | ||
| Body fat{{pmid|18597867}} | | Body fat{{pmid|18597867}} | ||
Line 1,215: | Line 1,326: | ||
| | | | ||
|- | |- | ||
| | |||
| Lean body mass{{pmid|17889950}}{{pmid|23642770}} | | Lean body mass{{pmid|17889950}}{{pmid|23642770}} | ||
| | | | ||
Line 1,220: | Line 1,332: | ||
| | | | ||
|- | |- | ||
| | |||
| | | | ||
| Soft lean mass{{pmid|22433233}} | | Soft lean mass{{pmid|22433233}} | ||
Line 1,226: | Line 1,339: | ||
|- | |- | ||
| Genetic index | | Genetic index | ||
| | |||
| | | | ||
| Terminal telomere restriction | | Terminal telomere restriction | ||
Line 1,233: | Line 1,347: | ||
|- | |- | ||
| Genetic index | | Genetic index | ||
| | |||
| | | | ||
| Terminal telomere restriction | | Terminal telomere restriction |
Revision as of 03:34, 3 February 2024
Biological Age (BA) is a concept used to assess an individual's aging status, offering a more nuanced understanding than Chronological Age (CA). Chronological age refers simply to the amount of time that has elapsed since a person's birth, while biological age provides a measure of aging based on various physiological, biochemical, and molecular factors. This distinction is crucial because individuals of the same chronological age can exhibit significantly different aging processes and health statuses.
Key Aspects of Biological Age
Biological age is estimated as the equivalent age within the same-sex population which corresponds to an individual's mortality risk.
- Biomarkers: Biological age is typically determined by analyzing a range of biomarkers. These can include genetic markers, epigenetic alterations, cellular senescence, telomere length, metabolic markers, and more. The specific biomarkers chosen depend on the method of estimation and the focus of the study.
- Health and Functionality: Biological age reflects the functional state of an individual's organs and systems. A lower biological age compared to chronological age might indicate better health and lower risk for age-related diseases, whereas a higher biological age suggests accelerated aging and potentially increased health risks.
- Variability: Unlike chronological age, which is uniform and progresses at a constant rate (one year per year), biological age can vary significantly between individuals. Factors such as lifestyle, genetics, environment, and disease can influence the rate at which a person's biological systems age. For example, biological age estimated from blood markers ranged between 20-years younger and 20-years older than individuals' chronological age.[1]
Importance in Research and Medicine
- Research Tool: In scientific research, biological age is valuable for understanding the aging process, identifying aging biomarkers, and evaluating the effectiveness of anti-aging interventions.
- Clinical Applications: In a clinical setting, biological age can be used to assess an individual's overall health status, predict the risk of age-related diseases, and personalize healthcare and treatment plans.
Biological Age Estimation Methods
Biological age estimation has emerged as a significant tool in gerontology, aiming to provide a more accurate measure of aging than chronological age.
The accurate estimation of biological age has significant implications for clinical practice, including predicting disease onset and prognosis, improving the quality of life for the elderly, and promoting successful aging. Each method offers unique insights, and a comprehensive understanding of these methods can lead to better clinical decision-making and more effective interventions for aging-related conditions.
Various methods have been developed to estimate biological age, each with its unique approach and criteria:[2]
- Multiple Linear Regression (MLR) is a statistical technique that estimates biological age by relating several independent variables (biomarkers) to a dependent variable (chronological age). In this method, chronological age is used as a criterion for selecting biomarkers and is treated as an independent index.
- Principal Component Analysis (PCA) is another statistical technique used in biological age estimation. PCA reduces the dimensionality of the data by transforming multiple biomarkers into a set of linearly uncorrelated variables, known as principal components.
- Hochschild’s Method differs from MLR and PCA by making chronological age an independent variable. It aims to estimate biological age by adjusting chronological age based on specific biomarkers.
- Klemera and Doubal’s Method (KDM) shares a similar concept with Hochschild’s method but uses a more complex statistical approach. It treats chronological age as an independent variable and incorporates multiple biomarkers to estimate biological age.
- Deep Learning-based approaches represent an emerging and powerful method for biological age estimation. Leveraging complex neural network architectures, these methods can analyze large datasets of biomarkers, integrating diverse types of biological data. Deep learning models can uncover intricate patterns in the data that may be missed by traditional statistical techniques, offering potentially more accurate and personalized biological age estimations. However, they require large, well-curated datasets to be effective.
Role of Chronological Age
The role of chronological age in the estimation of biological age varies significantly between different methods. In MLR and PCA, chronological age is used as a criterion for selecting biomarkers. This means that the biomarkers are chosen based on how well they correlate with chronological age. In this context, chronological age is not an independent variable in the statistical model but rather a reference point against which the predictive power of biomarkers is measured.
In contrast, Hochschild’s method and KDM treat chronological age as an independent variable. This means chronological age is directly incorporated into the model as one of the variables that predict biological age.
Comparison
Comparisons of various biological age estimation methods
Method | Proposed | Core concept | Advantage | Disadvantage |
---|---|---|---|---|
MLR | 1965, Hollingsworth[3] | Aging biomarkers are determined by the correlation with chronological age using MLR model |
|
|
PCA | 1988, Nakamura[7] | PCA uses fewer uncorrelated variables to explain the main variance |
| |
Hochschild’s method | 1989, Hochschild[9] | Hochschild’s method aims to select aging biomarkers according to their effects on life expectancy[9] |
|
|
KDM | 2006, Klemera and Doubal[8] | KDM is based on minimizing the distance between m regression lines and m biomarker points in an m-dimensional space of all biomarkers[8] |
| |
Deep learning | 2015[13] | Deep learning is a subfield of machine learning, where good features can be learned automatically using a general-purpose learning procedure[13]. Deep neural networks (DNNs)[14][15][16][17], convolutional neural networks (CNNs)[18][19], and recurrent neural networks (RNNs)[20] have been employed to build BA models in recent years. |
|
Biomarkers for Biological Age Estimation
Organ system | PCA | MLR | Hochschild’s | KDM |
---|---|---|---|---|
Cardiovascular system | Pulse pressure[21][22][23] | |||
Systolic blood pressure[7][24][25][26][27][28][29][12] | Systolic blood pressure[11][30][3][6][12] | Systolic blood pressure[12] | ||
Heart rate[7][24] | ||||
Intima-media thickness[21][31][22] | ||||
Maximum internal diameter of carotid artery[31][22] | ||||
End diastolic velocity[21] | ||||
Mitral valve annulus ventricular septum of the peak velocity of early filling[31] | ||||
Mitral valve annulus lateral wall of peak velocity of early filling[21] | ||||
Mitral annulus peak E anterior wall[22] | ||||
Ratio of peak velocity of early filling to atrial filling[21] | ||||
Respiratory system | VO2 max[32][26] | |||
Forced expiratory volume in 1 second[32][25][26][27][28] | Forced expiratory volume in 1 second[11][30][12] | Forced expiratory volume in 1 second[33] | Forced expiratory volume in 1 second[12] | |
Forced vital capacity[7][24][29] | Forced vital capacity[10] | Forced vital capacity[33] | ||
Maximal mid expiratory flow rate 75/25[31] | Vital capacity[3] | |||
Nervous system | Trail making test[31][23] | |||
Digital symbol test[10][22] | Digital symbol test[10] | |||
Memory test linking names with faces[10] | Memory test linking names with faces[10] | |||
Memory test: which picture is at what place[10] | Memory test: which picture is at what place[10] | |||
Speed test: pointing icons from 1 to 15 sequentially, mixed in random positions[10] | ||||
Visual reaction time[10][32] | Visual reaction time[33] | |||
Sequence of lamps[33] | ||||
Alternate button tapping time with/without decision[33] | ||||
Movement time with/without decision[33] | ||||
Renal system | Blood urea nitrogen[7][24][25][26][34][28][29] | Blood urea nitrogen[11][30][12] | Blood urea nitrogen[12] | |
Serum creatinine[12] | Serum creatinine[12] | |||
Cystatin C[21][31][22][23] | ||||
Liver | Serum albumin[25][26][34][28] | Serum albumin[6] | ||
Glutamic oxaloacetic transaminase[7][24] | Glutamic oxaloacetic transaminase[12] | Glutamic oxaloacetic transaminase[12] | ||
Glutamic pyruvic transaminase[29] | ||||
Ratio of albumin to globulin[27] | ||||
Lactate dehydrogenase[7][24][29] | ||||
Serum globulin[6] | ||||
Alkaline phosphatase[6] | ||||
Hematologic system | Erythrocyte sedimentation rate[26] | Erythrocyte sedimentation rate[6] | ||
Mean corpuscular hemoglobin[27] | ||||
Red blood cell count[28] | ||||
Hematocrit[25] | ||||
Hemoglobin concentration[7][24] | ||||
Fibrinogen[21] | ||||
Ferratin[12] | Ferratin[12] | |||
Metabolism | Glycosylated hemoglobin[26] | |||
Glucose[27][29] | Glucose[6] | |||
Low-density cholesterol[26] | ||||
Atherogenic index[7][24] | ||||
Triglyceride[24] | Triglycerides[30] | |||
Total cholesterol[29] | Total cholesterol[11][30][3][12] | Total cholesterol[12] | ||
Muscle and fat | Grip strength[10][32] | Grip strength[10][3] | ||
Soft lean mass[32] | ||||
Waist circumference[32][26] | Waist circumference[12] | Waist circumference[12] | ||
Percent body fat[26] | ||||
Sensory system | Hearing threshold[26] | |||
Highest audible pitch[10] | Highest audible pitch[10] | Highest audible pitch[33] | ||
Light extinction test[3] | ||||
Visual acuity[3] | ||||
Auditory function[3] | ||||
Vibrotactile sensitivity[3] | Vibrotactile sensitivity[33] | |||
Auditory reaction time[10] | Auditory reaction time[33] | |||
Focal range test using a Landolt ring[10] | Visual accommodation[33] | |||
Genetic index | Telomere restriction fragment[22] |
Biomarkers 2
The common aging biomarkers of four methods in different systems.
Here's a MediaWiki table format that includes only the biomarker column with their full names and abbreviations:
Biomarker |
---|
Systolic Blood Pressure (SBP) |
Diastolic Blood Pressure (DBP) |
Pulse Pressure |
Mean Arterial Pressure |
Pulse |
Pulse Wave Velocity |
Heart Rate |
Intima-Media Thickness |
Minimum Intima-Media Thickness |
End Diastolic Velocity |
Mitral Valve E/A Peak |
MVEL, MVES, MVEA |
Atherosclerosis Index |
NT-proBNP |
Cardiac Troponin I |
Creatine Phosphokinase |
Homocysteine |
Forced Vital Capacity (FVC) |
Forced Expiratory Volume in 1 Second (FEV1) |
Vital Capacity |
Maximal Midexpiratory Flow Rate 75/25 |
VO2 Max |
Chest Radiography |
Mini-Mental State Examination (MMSE) |
Digital Symbol Test |
Numeric Memory |
Associated Memory |
Topological Memory |
Short-Time Memory |
Concentration |
Intellectuality - Mental Defect |
Trail Making Test |
Glucose |
HBA1C |
C-peptide |
Insulin |
Triglyceride |
Total Cholesterol (TC) |
High-Density Lipoprotein (HDL), Low-Density Lipoprotein (LDL) |
Apolipoprotein A1 and B |
Thyroid-Stimulating Hormone (TSH) |
Testosterone |
Vitamin D |
Calcium |
Potassium |
Sodium |
Inorganic Phosphorus |
Urea |
Creatinine |
Estimated Glomerular Filtration Rate (eGFR) |
Uric Acid |
Cystatin C |
Creatinine Clearance |
Urine Specific Gravity |
Urine pH |
Alanine Aminotransferase (ALT) |
Aspartate Aminotransferase (AST) |
Alkaline Phosphatase (ALP) |
Total Protein |
Albumin |
Albumin/Globulin Ratio (A/G) |
Total Bilirubin |
Direct Bilirubin |
Amylase |
Lactate Dehydrogenase |
Alpha 2 Globulin |
Gamma Glutamyl Transpeptidase |
Red Blood Cell |
Red Blood Cell Volume Distribution Width |
Hematocrit |
Mean Corpuscular Volume |
Mean Corpuscular Hemoglobin |
Mean Corpuscular Hemoglobin Concentration |
Hemoglobin |
White Blood Cell |
Granulocytes |
Neutrophils |
Basophils, Eosinophils |
Lymphocytes |
Monocytes |
Platelet |
Mean Platelet Volume |
Platelet Distribution Width |
Erythrocyte Sedimentation Rate |
D-dimer, Fibrinogen |
Ferritin |
Transferrin |
Visual Accommodation |
Visual Reaction Time |
Visual Acuity |
Hearing |
Vibrotactile |
Retinal Photos |
C-Reactive Protein (CRP) |
Cytomegalovirus Optical Density |
Interleukin-6 |
P-selectin |
Grip Strength |
Vertical Jump |
Timed Up and Go Test |
Chair Rise Time |
1-Week Physical Activity |
Waist Circumference (WC) |
Waist-to-Hip Ratio |
Waist-to-Height Ratio |
Body Mass Index (BMI) |
Weight |
Height |
Body Fat |
Lean Body Mass |
Soft Lean Mass |
Terminal Telomere Restriction Fragment |
System | MLR | PCA | KDM | Deep learning | |
---|---|---|---|---|---|
Cardiovascular system | SBP[11][3][5][6][35][36][37][12][38] | SBP[11][5][7][24][29][39][27][25][28][26][32][12][38] | SBP[11][40][12][41][42][43][38][44][45][46] | ||
DBP[36][37][47] | DBP[47] | DBP[48][47] | |||
Pulse pressure[37] | Pulse pressure[23][31][21] | ||||
Mean arterial pressure[49] | |||||
Pulse[5] | Pulse[5][7] | ||||
Pulse wave velocity[35] | |||||
Heart rate[24] | |||||
Intima-media thickness[22][21] | |||||
Minimum intima-media | |||||
End diastolic velocity[21] | |||||
mitral valve E/A peak[23][21] | |||||
MVEL[21], MVES[31], MVEA[22] | |||||
Atherosclerosis index[7][24] | |||||
NT-proBNP[17] | |||||
Cardiac troponin I[17] | |||||
Creatine phosphokinase[37] | |||||
Homocysteine[37] | |||||
Respiratory
system |
FVC[5][36][37][10] | FVC[5][7][24][29][39] | FVC[10] | ||
FEV1[11][6][50][36][37][12][38][47] | FEV1[11][39][27][25][28][26][32][12][38][47] | FEV1[11][40][12][41][42][38][47] | |||
Vital capacity[3][35] | |||||
Maximal midexpiratory
flow rate 75/25[31] |
|||||
VO2 max[26][32] | |||||
Chest radiography[19] | |||||
Nervous system | MMSE[47] | MMSE[47] | MMSE[47] | ||
Digital symbol test[35] | Digital symbol test[22] | ||||
Numeric memory[10] | Numeric memory[10] | ||||
Associated memory[10] | Associated memory[10] | ||||
Topological memory[10] | Topological memory[10] | ||||
Short-time memory[51] | |||||
Concentration[10] | Concentration[10] | ||||
Intellectuality -mental defect[35] | |||||
Trail making test[23][31] | |||||
Endocrine metabolic system | Glucose[36][37] | Glucose[29][27][49] | Glucose[42] | Glucose[14][15][16][17] | |
HBA1C[11][37] | HBA1C[11][26] | HBA1C[11][40][41][43][44][45][52][46] | HBA1C[16] | ||
C-peptide[17] | |||||
Insulin[17] | |||||
Triglyceride[6][36][37] | Triglyceride[24][49] | Triglyceride[45] | Triglyceride[15][17] | ||
TC[11][3][5][6][50][36][37][12] | TC[11][5][29][12] | TC[11][40][12][41][42][44][45][46] | TC[14][15] | ||
HDL[36], LDL[37] | HDL[49], LDL[26] | HDL[15][17],LDL[15][17] | |||
Apolipoprotein A1 and B[17] | |||||
TSH[36] | TSH[48] | ||||
Testosterone[36] | Testosterone[17] | ||||
Vitamin D[38] | Vitamin D[38] | Vitamin D[38] | Vitamin D[17] | ||
Calcium[48] | Calcium[15] | ||||
Potassium[15] | |||||
Sodium[15] | |||||
Inorganic phosphorus[48] | |||||
Urinary system | Urea[11][5][6][37][12] | Urea[11][5][7][24][29][39][25][28][26][12] | Urea[11][40][48][12][43][44][45][52] | Urea[14][15][16] | |
Creatinine[11][36][37][12][38] | Creatinine[12][38] | Creatinine[11][40][48][41][43][44][45][52][46] | Creatinine[15][17] | ||
eGFR[47] | eGFR[47] | eGFR[47] | |||
Uric acid[43][52] | Uric acid[17] | ||||
Cystatin C[23][22][31][21] | Cystatin C[17] | ||||
Creatinine clearance[37] | |||||
Urine specific gravity[37] | |||||
Urine pH[37] | |||||
Digestive system | ALT[37] | ALT[29] | ALT[17] | ||
AST[5][37][12] | AST[5][7][24][12] | AST[12] | AST[17] | ||
ALP[11][6][37] | ALP[11] | ALP[11][40][48][41][43][52][46] | ALP[14] | ||
Total protein[37] | Total protein[48] | Total protein[15] | |||
Albumin[11][5][37] | Albumin[11][5][39][25][28][26] | Albumin[11][40][48][41][43][44][45][52][46] | Albumin[14][15][17] | ||
A/G[5][37] | A/G[5][39][27] | ||||
Total bilirubin[37] | Total bilirubin[15] | ||||
Direct bilirubin[37] | |||||
Amylase[37] | |||||
Lactate dehydrogenase[50][37] | Lactate dehydrogenase[24][29] | ||||
Alpha 2 globulin[14] | |||||
Gamma glutamyl
transpeptidase[37] |
|||||
Hematologic System | Red blood cell[38] | Red blood cell[39][28][38] | Red blood cell[38][45] | Red blood cell[14][15][17] | |
Red blood cell volume
distribution width[43] |
Red blood cell volume | ||||
Hematocrit[39][25] | Hematocrit[14][15] | ||||
Mean corpuscular | Mean corpuscular | ||||
Mean corpuscular
hemoglobin[27] |
|||||
Mean corpuscular hemoglobin concentration[15][17] | |||||
Hemoglobin[5][47] | Hemoglobin[5][7][24][29][39][47] | Hemoglobin[48][47] | Hemoglobin[15][17] | ||
White blood cell[43][44][52] | White blood cell[17] | ||||
Granulocytes[17] | |||||
Neutrophils[17] | |||||
Basophils[17], Eosinophils[17] | |||||
Lymphocytes[43][44][52] | Lymphocytes[14][17] | ||||
Monocytes[47] | Monocytes[47] | Monocytes[47] | Monocytes[17] | ||
Platelet[45] | Platelet[15][17] | ||||
Mean platelet volume[17] | |||||
Platelet distribution width[17] | |||||
Erythrocyte | Erythrocyte | ||||
sedimentation rat[6][36] | sedimentation rat[26] | ||||
D-dimer[22]
Fibrinogen[21] |
D-dimer[17] | ||||
Ferritin[12] | Ferritin[12] | Ferritin[12][45] | Ferritin[16] | ||
Fransferrin[45] | |||||
Sensory system | Visual accommodation[35][10] | Visual accommodation[10] | |||
Visual reaction time[10] | Visual reaction time[10] | ||||
Visual acuity[3][5] | Visual acuity[5] | ||||
Hearing[3][50][35][10] | Hearing[26] | Hearing[10] | |||
Vibrotactile[3][51][10] | Vibrotactile[10] | ||||
Retinal photos | |||||
Inflammatory index | CRP[11] | CRP[11] | CRP[11][40][41][42][43][44][45][52][46] | CRP[17] | |
Cytomegalovirus optical density[11] | Cytomegalovirus
optical density[11] |
Cytomegalovirus | |||
Interleukin-6[42] | |||||
P-selectin[42] | |||||
Motion index | Grip strength[3][51][47][10] | Grip strength[32][47] | Grip strength[47][10] | ||
Vertical jump[32] | |||||
Timed up and go test[47] | Timed up and go test[47] | Timed up and go test[47] | |||
Chair rise time[47] | Chair rise time[47] | Chair rise time[47] | |||
1-week physical activity[18][20] | |||||
Body morphology index | WC[37][12] | WC[26][32][12][49] | WC[12] | ||
Waist-to-hip ratio[36][37] | |||||
Waist-to-height ratio[38] | Waist-to-height ratio[38] | Waist-to-height ratio[38] | |||
Body mass index[36][37] | |||||
Weight[35] | |||||
Height[47] | Height[47] | Height[47] | |||
Body fat[36][37] | Body fat[26] | ||||
Lean body mass[36][37] | |||||
Soft lean mass[32] | |||||
Genetic index | Terminal telomere restriction
fragment[22] |
||||
Genetic index | Terminal telomere restriction
fragment[22] |
SBP, systolic blood pressure; DBP, diastolic blood pressure; NT-proBNP, N-terminal pro brain natriuretic peptide; MVEA, mitral annulus peak E anterior wall; MVEL, mitral valve annulus lateral wall of peak velocity of early filling; MVES, mitral valve annulus ventricular septum of the peak velocity of early filling; FEV1, forced expiratory volume in 1.0 s; FVC, forced vital capacity; MMSE, mini-mental state examination; eGFR, estimated glomerular filtration rat; HBA1C, glycosylated hemoglobin; HDL, high density lipoprotein; LDL, low density lipoprotein; TSH, thyroid stimulating hormone; ALT, Alanine aminotransferase; AST, Aspartate aminotransferase; ALP, alkaline phosphatase; A/G, ratio of albumin to globulin; CRP, c-reactive protein; WC, waist circumference.
Further Reading
- 2017, Common methods of biological age estimation [2]
- 2023, Progress in biological age research [53]
Todo
- 2017, Biological Age Predictors [54]
- 2022, Biological Age Predictors: The Status Quo and Future Trends [55]
- 2021, Predictors of Biological Age: The Implications for Wellness and Aging Research [56]
- 2023, Biological age estimation using circulating blood biomarkers [1]
- 2021, Deep learning for biological age estimation [57]
See Also
- Epigenetic Clocks
- Wikipedia - Biomarkers of aging
References
- ↑ 1.0 1.1 Bortz J et al.: Biological age estimation using circulating blood biomarkers. Commun Biol 2023. (PMID 37884697) [PubMed] [DOI] [Full text] Biological age captures physiological deterioration better than chronological age and is amenable to interventions. Blood-based biomarkers have been identified as suitable candidates for biological age estimation. This study aims to improve biological age estimation using machine learning models and a feature-set of 60 circulating biomarkers available from the UK Biobank (n = 306,116). We implement an Elastic-Net derived Cox model with 25 selected biomarkers to predict mortality risk (C-Index = 0.778; 95% CI [0.767-0.788]), which outperforms the well-known blood-biomarker based PhenoAge model (C-Index = 0.750; 95% CI [0.739-0.761]), providing a C-Index lift of 0.028 representing an 11% relative increase in predictive value. Importantly, we then show that using common clinical assay panels, with few biomarkers, alongside imputation and the model derived on the full set of biomarkers, does not substantially degrade predictive accuracy from the theoretical maximum achievable for the available biomarkers. Biological age is estimated as the equivalent age within the same-sex population which corresponds to an individual's mortality risk. Values ranged between 20-years younger and 20-years older than individuals' chronological age, exposing the magnitude of ageing signals contained in blood markers. Thus, we demonstrate a practical and cost-efficient method of estimating an improved measure of Biological Age, available to the general population.
- ↑ 2.0 2.1 Jia L et al.: Common methods of biological age estimation. Clin Interv Aging 2017. (PMID 28546743) [PubMed] [DOI] [Full text] At present, no single indicator could be used as a golden index to estimate aging process. The biological age (BA), which combines several important biomarkers with mathematical modeling, has been proposed for >50 years as an aging estimation method to replace chronological age (CA). The common methods used for BA estimation include the multiple linear regression (MLR), the principal component analysis (PCA), the Hochschild's method, and the Klemera and Doubal's method (KDM). The fundamental differences in these four methods are the roles of CA and the selection criteria of aging biomarkers. In MLR and PCA, CA is treated as the selection criterion and an independent index. The Hochschild's method and KDM share a similar concept, making CA an independent variable. Previous studies have either simply constructed the BA model by one or compared the four methods together. However, reviews have yet to illustrate and compare the four methods systematically. Since the BA model is a potential estimation of aging for clinical use, such as predicting onset and prognosis of diseases, improving the elderly's living qualities, and realizing successful aging, here we summarize previous BA studies, illustrate the basic statistical steps, and thoroughly discuss the comparisons among the four common BA estimation methods.
- ↑ 3.00 3.01 3.02 3.03 3.04 3.05 3.06 3.07 3.08 3.09 3.10 3.11 3.12 3.13 3.14 3.15 Hollingsworth JW et al.: Correlations between tests of aging in Hiroshima subjects--an attempt to define "physiologic age". Yale J Biol Med 1965. (PMID 5841151) [PubMed] [Full text]
- ↑ Dubina TL et al.: Biological age and its estimation. II. Assessment of biological age of albino rats by multiple regression analysis. Exp Gerontol 1983. (PMID 6873212) [PubMed] [DOI] Multiple regression model of biological age (BA) theoretically gives agreement with the main concept of BA. When assessment of BA is based on the model, the age being in regression center, the method provides satisfactory results, whereas BA estimates of individuals in extreme age groups are erroneous. Investigation of male and female Wistar rats of age 5-29 months showed the BA estimates calculated from 4-10 physiological indices in young (5-7 mo) animals are overestimated, and in old (24-28 mo) animals are underestimated. Coincidence of average BA in one-age group of animals with its chronological age served as a criterion for the correspondence of the estimate to "real" BA. The paper also examines the following questions: the necessary and sufficient number of physiological indices; the sample size from the intact animal population to establish normal aging standard; the relationship between BA and animal weight.
- ↑ 5.00 5.01 5.02 5.03 5.04 5.05 5.06 5.07 5.08 5.09 5.10 5.11 5.12 5.13 5.14 5.15 5.16 5.17 5.18 5.19 5.20 5.21 Nakamura E et al.: Assessment of biological age by principal component analysis. Mech Ageing Dev 1988. (PMID 3226152) [PubMed] [DOI] A method of assessing biological age by the application of principal component analysis is reported. Healthy individuals (462) randomly selected from about 6000 men who had taken a 2-day health examination were studied. Out of the 30 physiological variables examined in routine check-ups, 11 variables were selected as suitable for the assessment of biological age based on the results of factor analysis and the physiological meaning of each test. This variable set was then submitted to principal component analysis, and the 1st principal component obtained from this analysis was used as an equation for assessing one's biological age. However, the biological age calculated from this equation is expressed as a score, so the estimated score was transformed to years (biological age) using the T-score idea. The biological age estimated by this method is practically useful and theoretically valid in contrast with the multiple regression model, because this approach eliminates and overcomes the following 2 big problems of the multiple regression model: (1) the distortion of the individual biological age at the regression edges; and (2) a theoretical contradiction in that a perfect model will merely be predicting the subject's chronological age, not his biological age.
- ↑ 6.00 6.01 6.02 6.03 6.04 6.05 6.06 6.07 6.08 6.09 6.10 6.11 6.12 6.13 Webster IW & Logie AR: A relationship between functional age and health status in female subjects. J Gerontol 1976. (PMID 950448) [PubMed] [DOI] A multiple regression equation was used to predict age from seven clinical variables in 1080 apparently well female subjects. A multiple correlation coefficient of R = 0.77 was achieved by five of the variables: timed forced expiratory volume, systolic blood pressure, plasma urea nitrogen, cholesterol, and alkaline phosphatase. On the basis of selection by medical questionnaire responses and other objective criteria, 9% of the subjects were nonsmokers and healthier than the rest. These selected subjects showed a significant reduction in preducted age. Within this group, subjective perception of health was associated with differences in predicted age: poor health with an increase and good health with a decrease in functional age. This study of functional age was based on the healthiest segment of the population in order to minimize the effect of overt pathological processes on the aging rate. An association has been demonstrated between health impairment and predicted age as a measure of the aging rate.
- ↑ 7.00 7.01 7.02 7.03 7.04 7.05 7.06 7.07 7.08 7.09 7.10 7.11 7.12 7.13 7.14 7.15 Nakamura E et al.: Biological age versus physical fitness age. Eur J Appl Physiol Occup Physiol 1989. (PMID 2737197) [PubMed] [DOI] A population of healthy middle-aged (n = 69) and elderly men (n = 12), who participated in a health promotion program, was studied to determine whether really physically fit individuals are in good biological condition, and also whether improvement of physical fitness in the middle-aged and the elderly reduces their "rate of aging". Biological and physical fitness ages of the individuals studied were estimated from the data for 18 physiological function tests and 5 physical fitness tests, respectively, by a principal component model. The correlation coefficient between the estimated biological and physical fitness ages was 0.72 (p less than 0.01). Detailed analyses of the relationship between the estimated biological and physical fitness ages revealed that those who manifested a higher ("older") physical fitness age did not necessarily have a higher biological age, but those who manifested a lower ("younger") physical fitness age were also found to have a lower biological age. These results suggested that there were considerable individual variations in the relationship between biological condition and physical fitness among individuals with an old physical fitness age, but those who were in a state of high physical fitness maintained a relatively good biological condition. The data regarding the elderly men who had maintained a regular exercise program indicated that their estimated biological ages were considerably younger than the expected values. This might suggest that in older individuals regular physical activity may provide physiological improvements which in turn might reduce "the rate of aging".
- ↑ 8.0 8.1 8.2 8.3 Klemera P & Doubal S: A new approach to the concept and computation of biological age. Mech Ageing Dev 2006. (PMID 16318865) [PubMed] [DOI] The lack of exact definition of the concept of biological age (BA) is a typical feature of works concerning BA. That is why comparison of results of various published methods makes little sense and eventual proof of their optimality is impossible. Based on natural and simple presumptions, an attempt to express mathematically the supposed relation between chronological age (CA) and BA has proven to be unexpectedly fruitful. In the present paper, an optimum method of estimation of BA, which is easily applicable even in nonlinear cases, is derived. Moreover, the method allows evaluating the precision of the estimates and also offers tools for validation of presumptions of the method. A special feature of the method is that CA should be used as a standard biomarker, leading to essential improving the precision of BA-estimate and illuminating relativity of the known "paradox of biomarkers". All theoretical results of the method were fully approved by means of a special simulation program. Further, the theory and the results of the simulation have proven that many published results of BA-estimates using multiple linear regression (MLR) are very probably disserviceable because CA is typically more precise estimate of BA than estimates computed by MLR. This unpleasant conclusion also concerns methods, which use MLR as the final step after transformation of the battery of biomarkers by factor analysis or by principal component analysis.
- ↑ 9.0 9.1 Hochschild R: Improving the precision of biological age determinations. Part 1: A new approach to calculating biological age. Exp Gerontol 1989. (PMID 2684676) [PubMed] [DOI] In calculating biological age, almost all prior studies used multiple regression of chronological age on scores of biomarkers of aging. Multiple regression is invalid for this purpose for three, and in some circumstances four, reasons. These are: a) weighting of the contribution of each biomarker's scores according to strength of association with chronological age; b) regression of calculated ages to sample mean age and the inadequacy of proposed corrections; c) frequent occurrence of regression coefficients whose sign equates poorer adult performance on a test to younger biological ages; and d) multicollinearity when lung function scores and height are on the same side of the regression equation. An alternative method for calculating biological age is outlined. Regression to sample mean age and its solution are illustrated on data for highest audible pitch, one of 12 biomarkers measured in a study of 2462 office workers. Prior published studies employing multiple regression to calculate biological age appear to have been in error.
- ↑ 10.00 10.01 10.02 10.03 10.04 10.05 10.06 10.07 10.08 10.09 10.10 10.11 10.12 10.13 10.14 10.15 10.16 10.17 10.18 10.19 10.20 10.21 10.22 10.23 10.24 10.25 10.26 10.27 10.28 10.29 10.30 10.31 10.32 10.33 10.34 10.35 10.36 10.37 10.38 Cho IH et al.: An empirical comparative study on biological age estimation algorithms with an application of Work Ability Index (WAI). Mech Ageing Dev 2010. (PMID 20005245) [PubMed] [DOI] In this study, we described the characteristics of five different biological age (BA) estimation algorithms, including (i) multiple linear regression, (ii) principal component analysis, and somewhat unique methods developed by (iii) Hochschild, (iv) Klemera and Doubal, and (v) a variant of Klemera and Doubal's method. The objective of this study is to find the most appropriate method of BA estimation by examining the association between Work Ability Index (WAI) and the differences of each algorithm's estimates from chronological age (CA). The WAI was found to be a measure that reflects an individual's current health status rather than the deterioration caused by a serious dependency with the age. Experiments were conducted on 200 Korean male participants using a BA estimation system developed principally under the concept of non-invasive, simple to operate and human function-based. Using the empirical data, BA estimation as well as various analyses including correlation analysis and discriminant function analysis was performed. As a result, it had been confirmed by the empirical data that Klemera and Doubal's method with uncorrelated variables from principal component analysis produces relatively reliable and acceptable BA estimates.
- ↑ 11.00 11.01 11.02 11.03 11.04 11.05 11.06 11.07 11.08 11.09 11.10 11.11 11.12 11.13 11.14 11.15 11.16 11.17 11.18 11.19 11.20 11.21 11.22 11.23 11.24 11.25 11.26 11.27 11.28 11.29 11.30 11.31 11.32 11.33 11.34 11.35 Levine ME: Modeling the rate of senescence: can estimated biological age predict mortality more accurately than chronological age?. J Gerontol A Biol Sci Med Sci 2013. (PMID 23213031) [PubMed] [DOI] [Full text] Biological age (BA) is useful for examining differences in aging rates. Nevertheless, little consensus exists regarding optimal methods for calculating BA. The aim of this study is to compare the predictive ability of five BA algorithms. The sample included 9,389 persons, aged 30-75 years, from National Health and Nutrition Examination Survey III. During the 18-year follow-up, 1,843 deaths were counted. Each BA algorithm was compared with chronological age on the basis of predictive sensitivity and strength of association with mortality. Results found that the Klemera and Doubal method was the most reliable predictor of mortality and performed significantly better than chronological age. Furthermore, when included with chronological age in a model, Klemera and Doubal method had more robust predictive ability and caused chronological age to no longer be significantly associated with mortality. Given the potential of BA to highlight heterogeneity, the Klemera and Doubal method algorithm may be useful for studying a number of questions regarding the biology of aging.
- ↑ 12.00 12.01 12.02 12.03 12.04 12.05 12.06 12.07 12.08 12.09 12.10 12.11 12.12 12.13 12.14 12.15 12.16 12.17 12.18 12.19 12.20 12.21 12.22 12.23 12.24 12.25 12.26 12.27 12.28 12.29 12.30 12.31 12.32 12.33 12.34 12.35 12.36 12.37 12.38 12.39 12.40 Jee H & Park J: Selection of an optimal set of biomarkers and comparative analyses of biological age estimation models in Korean females. Arch Gerontol Geriatr 2017. (PMID 28110151) [PubMed] [DOI] To date, an optimal working model which predicts biological age (BA) with a set of working biomarkers has not been devised to represent the Korean female population. Accuracy of prediction and applicability are required of an optimal set of commonly assessed biomarkers to provide information on the health status. The goal of this study was to identify a set of biomarkers that represent the aging process and to develop and compare different BA prediction models to elucidate the most fitting and applicable model for providing information on health status in the Korean female population. Using a series of selection processes, eight clinically assessable variables were selected by analyzing relations between 31 clinical variables and chronologic age in 912 normal, healthy individuals among 3642 female participants with ages ranging from 30 to 80 years. The multiple linear regression (MLR), principal component analysis (PCA), and the Klemera-Doubal (KDM) statistical methods were applied to obtain three different sets of BA prediction models. These three models were assessed by calculating and performing the coefficient determinations (r2), regression slopes, effect sizes, pairwise t-tests, and Bland-Altman plots. The BA models were further compared for the applicability by calculating the BAs of clinical risk groups. MLR showed the narrowing effects at the either ends of the age spectrum with greatest effect sizes. PCA showed the greatest degree of dispersion and deviation from the regression center. These MLR and PCA trends were also exhibited by clinically risk groups. In conclusion, the KDM BA prediction model based on the selected biomarkers was found to provide the most reliable and stable results for the practical assessment of BA.
- ↑ 13.0 13.1 13.2 13.3 LeCun Y et al.: Deep learning. Nature 2015. (PMID 26017442) [PubMed] [DOI] Deep learning allows computational models that are composed of multiple processing layers to learn representations of data with multiple levels of abstraction. These methods have dramatically improved the state-of-the-art in speech recognition, visual object recognition, object detection and many other domains such as drug discovery and genomics. Deep learning discovers intricate structure in large data sets by using the backpropagation algorithm to indicate how a machine should change its internal parameters that are used to compute the representation in each layer from the representation in the previous layer. Deep convolutional nets have brought about breakthroughs in processing images, video, speech and audio, whereas recurrent nets have shone light on sequential data such as text and speech.
- ↑ 14.00 14.01 14.02 14.03 14.04 14.05 14.06 14.07 14.08 14.09 14.10 14.11 Putin E et al.: Deep biomarkers of human aging: Application of deep neural networks to biomarker development. Aging (Albany NY) 2016. (PMID 27191382) [PubMed] [DOI] [Full text] One of the major impediments in human aging research is the absence of a comprehensive and actionable set of biomarkers that may be targeted and measured to track the effectiveness of therapeutic interventions. In this study, we designed a modular ensemble of 21 deep neural networks (DNNs) of varying depth, structure and optimization to predict human chronological age using a basic blood test. To train the DNNs, we used over 60,000 samples from common blood biochemistry and cell count tests from routine health exams performed by a single laboratory and linked to chronological age and sex. The best performing DNN in the ensemble demonstrated 81.5 % epsilon-accuracy r = 0.90 with R(2) = 0.80 and MAE = 6.07 years in predicting chronological age within a 10 year frame, while the entire ensemble achieved 83.5% epsilon-accuracy r = 0.91 with R(2) = 0.82 and MAE = 5.55 years. The ensemble also identified the 5 most important markers for predicting human chronological age: albumin, glucose, alkaline phosphatase, urea and erythrocytes. To allow for public testing and evaluate real-life performance of the predictor, we developed an online system available at http://www.aging.ai. The ensemble approach may facilitate integration of multi-modal data linked to chronological age and sex that may lead to simple, minimally invasive, and affordable methods of tracking integrated biomarkers of aging in humans and performing cross-species feature importance analysis.
- ↑ 15.00 15.01 15.02 15.03 15.04 15.05 15.06 15.07 15.08 15.09 15.10 15.11 15.12 15.13 15.14 15.15 15.16 15.17 15.18 15.19 Mamoshina P et al.: Population Specific Biomarkers of Human Aging: A Big Data Study Using South Korean, Canadian, and Eastern European Patient Populations. J Gerontol A Biol Sci Med Sci 2018. (PMID 29340580) [PubMed] [DOI] [Full text] Accurate and physiologically meaningful biomarkers for human aging are key to assessing antiaging therapies. Given ethnic differences in health, diet, lifestyle, behavior, environmental exposures, and even average rate of biological aging, it stands to reason that aging clocks trained on datasets obtained from specific ethnic populations are more likely to account for these potential confounding factors, resulting in an enhanced capacity to predict chronological age and quantify biological age. Here, we present a deep learning-based hematological aging clock modeled using the large combined dataset of Canadian, South Korean, and Eastern European population blood samples that show increased predictive accuracy in individual populations compared to population specific hematologic aging clocks. The performance of models was also evaluated on publicly available samples of the American population from the National Health and Nutrition Examination Survey (NHANES). In addition, we explored the association between age predicted by both population specific and combined hematological clocks and all-cause mortality. Overall, this study suggests (a) the population specificity of aging patterns and (b) hematologic clocks predicts all-cause mortality. The proposed models were added to the freely-available Aging.AI system expanding the range of tools for analysis of human aging.
- ↑ 16.0 16.1 16.2 16.3 16.4 Mamoshina P et al.: Blood Biochemistry Analysis to Detect Smoking Status and Quantify Accelerated Aging in Smokers. Sci Rep 2019. (PMID 30644411) [PubMed] [DOI] [Full text] There is an association between smoking and cancer, cardiovascular disease and all-cause mortality. However, currently, there are no affordable and informative tests for assessing the effects of smoking on the rate of biological aging. In this study we demonstrate for the first time that smoking status can be predicted using blood biochemistry and cell count results andthe recent advances in artificial intelligence (AI). By employing age-prediction models developed using supervised deep learning techniques, we found that smokers exhibited higher aging rates than nonsmokers, regardless of their cholesterol ratios and fasting glucose levels. We further used those models to quantify the acceleration of biological aging due to tobacco use. Female smokers were predicted to be twice as old as their chronological age compared to nonsmokers, whereas male smokers were predicted to be one and a half times as old as their chronological age compared to nonsmokers. Our findings suggest that deep learning analysis of routine blood tests could complement or even replace the current error-prone method of self-reporting of smoking status and could be expanded to assess the effect of other lifestyle and environmental factors on aging.
- ↑ 17.00 17.01 17.02 17.03 17.04 17.05 17.06 17.07 17.08 17.09 17.10 17.11 17.12 17.13 17.14 17.15 17.16 17.17 17.18 17.19 17.20 17.21 17.22 17.23 17.24 17.25 17.26 17.27 17.28 17.29 17.30 17.31 17.32 17.33 17.34 Gialluisi A et al.: Exploring domains, clinical implications and environmental associations of a deep learning marker of biological ageing. Eur J Epidemiol 2022. (PMID 34453631) [PubMed] [DOI] Deep Neural Networks (DNN) have been recently developed for the estimation of Biological Age (BA), the hypothetical underlying age of an organism, which can differ from its chronological age (CA). Although promising, these population-specific algorithms warrant further characterization and validation, since their biological, clinical and environmental correlates remain largely unexplored. Here, an accurate DNN was trained to compute BA based on 36 circulating biomarkers in an Italian population (N = 23,858; age ≥ 35 years; 51.7% women). This estimate was heavily influenced by markers of metabolic, heart, kidney and liver function. The resulting Δage (BA-CA) significantly predicted mortality and hospitalization risk for all and specific causes. Slowed biological aging (Δage < 0) was associated with higher physical and mental wellbeing, healthy lifestyles (e.g. adherence to Mediterranean diet) and higher socioeconomic status (educational attainment, household income and occupational status), while accelerated aging (Δage > 0) was associated with smoking and obesity. Together, lifestyles and socioeconomic variables explained ~48% of the total variance in Δage, potentially suggesting the existence of a genetic basis. These findings validate blood-based biological aging as a marker of public health in adult Italians and provide a robust body of knowledge on its biological architecture, clinical implications and potential environmental influences.
- ↑ 18.0 18.1 Pyrkov TV et al.: Extracting biological age from biomedical data via deep learning: too much of a good thing?. Sci Rep 2018. (PMID 29581467) [PubMed] [DOI] [Full text] Age-related physiological changes in humans are linearly associated with age. Naturally, linear combinations of physiological measures trained to estimate chronological age have recently emerged as a practical way to quantify aging in the form of biological age. In this work, we used one-week long physical activity records from a 2003-2006 National Health and Nutrition Examination Survey (NHANES) to compare three increasingly accurate biological age models: the unsupervised Principal Components Analysis (PCA) score, a multivariate linear regression, and a state-of-the-art deep convolutional neural network (CNN). We found that the supervised approaches produce better chronological age estimations at the expense of a loss of the association between the aging acceleration and all-cause mortality. Consequently, we turned to the NHANES death register directly and introduced a novel way to train parametric proportional hazards models suitable for out-of-the-box implementation with any modern machine learning software. As a demonstration, we produced a separate deep CNN for mortality risks prediction that outperformed any of the biological age or a simple linear proportional hazards model. Altogether, our findings demonstrate the emerging potential of combined wearable sensors and deep learning technologies for applications involving continuous health risk monitoring and real-time feedback to patients and care providers.
- ↑ 19.0 19.1 Raghu VK et al.: Deep Learning to Estimate Biological Age From Chest Radiographs. JACC Cardiovasc Imaging 2021. (PMID 33744131) [PubMed] [DOI] OBJECTIVES: The goal of this study was to assess whether a deep learning estimate of age from a chest radiograph image (CXR-Age) can predict longevity beyond chronological age. BACKGROUND: Chronological age is an imperfect measure of longevity. Biological age, a measure of overall health, may improve personalized care. This paper proposes a new way to estimate biological age using a convolutional neural network that takes as input a CXR image and outputs a chest x-ray age (in years) as a measure of long-term mortality risk. METHODS: CXR-Age was developed using CXR from 116,035 individuals and validated in 2 held-out testing sets: 1) 75% of the CXR arm of PLCO (Prostate, Lung, Colorectal, and Ovarian Cancer Screening Trial) (N = 40,967); and 2) the CXR arm of NLST (National Lung Screening Trial) (N = 5,414). CXR-Age was compared to chronological age and a multivariable regression model of chronological age, risk factors, and radiograph findings to predict all-cause and cardiovascular mortality with a maximum 23 years and 13 years of follow-up, respectively. The primary outcome was observed mortality; results are provided for the testing datasets only. RESULTS: In the PLCO testing dataset, a 5-year increase in CXR-Age carried a higher risk of all-cause mortality than a 5-year increase in chronological age (CXR-Age hazard ratio [HR]: 2.26 [95% confidence interval (CI): 2.24 to 2.29] vs. chronological age HR: 1.77 [95% CI: 1.75 to 1.78]; p < 0.001). A similar pattern was found for cardiovascular mortality (CXR-Age cause-specific HR: 2.45 per 5 years [95% CI: 2.34 to 2.56] vs. chronological age HR: 1.82 per 5 years [95% CI: 1.74 to 1.90]). Similar results were seen for both outcomes in the NLST external testing dataset. Adding CXR-Age to the multivariable model resulted in significant improvements for predicting both outcomes in both testing datasets (p < 0.001 for all comparisons). CONCLUSIONS: Based on a CXR image, CXR-Age predicted long-term all-cause and cardiovascular mortality.
- ↑ 20.0 20.1 Rahman SA & Adjeroh DA: Deep Learning using Convolutional LSTM estimates Biological Age from Physical Activity. Sci Rep 2019. (PMID 31388024) [PubMed] [DOI] [Full text] Human age estimation is an important and difficult challenge. Different biomarkers and numerous approaches have been studied for biological age estimation, each with its advantages and limitations. In this work, we investigate whether physical activity can be exploited for biological age estimation for adult humans. We introduce an approach based on deep convolutional long short term memory (ConvLSTM) to predict biological age, using human physical activity as recorded by a wearable device. We also demonstrate five deep biological age estimation models including the proposed approach and compare their performance on the NHANES physical activity dataset. Results on mortality hazard analysis using both the Cox proportional hazard model and Kaplan-Meier curves each show that the proposed method for estimating biological age outperforms other state-of-the-art approaches. This work has significant implications in combining wearable sensors and deep learning techniques for improved health monitoring, for instance, in a mobile health environment. Mobile health (mHealth) applications provide patients, caregivers, and administrators continuous information about a patient, even outside the hospital.
- ↑ 21.00 21.01 21.02 21.03 21.04 21.05 21.06 21.07 21.08 21.09 21.10 21.11 21.12 21.13 Bai X et al.: Evaluation of biological aging process - a population-based study of healthy people in China. Gerontology 2010. (PMID 19940465) [PubMed] [DOI] BACKGROUND: Although there have been cross-sectional and longitudinal studies examining biological age (BA) with chronological age (CA)-related changes in physical, physiological, biochemical, and hormonal variables, few studies have performed echocardiographic evaluation of the cardiovascular system and inflammatory biomarkers. Furthermore, little is known about biomarkers of aging and BA score (BAS) for healthy people in China. OBJECTIVES: The purpose of this study was to identify the biomarkers of healthy aging and to establish BAS for healthy people in China. METHODS: We examined 2,876 men and women aged 30-98 years old in three Chinese cities, and 852 healthy subjects were assessed with 108 physical, morphological, physiological and biochemical variables. After excluding binary variables, variables that had a correlation coefficient with CA of < or =0.25 and redundant variables, eight variables including CA, arterial pulse pressure (PP), intima-media thickness (IMT), end diastolic velocity (EDV), ratio of peak velocity of early filling to atrial filling (E/A), mitral valve annulus lateral wall of peak velocity of early filling (MVEL), cystatin C (CYSC), and fibrinogen (FIB) were selected as candidate biomarkers of aging based on a factor-weighted BAS composite for predicting BA. RESULTS: The BAS equation was 0.248 (CA) + 0.195 (IMT) - 0.196 (EDV) - 0.167 (E/A) - 0.166 (MVEL) + 0.188 (PP) + 0.182 (FIB) + 0.193 (CYSC). Individual BAS were significantly correlated with CA (r = 0.893, p < 0.001). Biological aging rate predicted by BAS was accelerated with increases in CA, and peaked when healthy men and women reached > or =75 years of age. CONCLUSIONS: Our data suggest that BAS is superior to CA in assessing the rate of aging in healthy Chinese people. The cardiovascular variables play a crucial role in the evaluation of biological aging. Biological aging rate appears to be age specific.
- ↑ 22.00 22.01 22.02 22.03 22.04 22.05 22.06 22.07 22.08 22.09 22.10 22.11 22.12 22.13 Zhang WG et al.: Select aging biomarkers based on telomere length and chronological age to build a biological age equation. Age (Dordr) 2014. (PMID 24659482) [PubMed] [DOI] [Full text] The purpose of this study is to build a biological age (BA) equation combining telomere length with chronological age (CA) and associated aging biomarkers. In total, 139 healthy volunteers were recruited from a Chinese Han cohort in Beijing. A genetic index, renal function indices, cardiovascular function indices, brain function indices, and oxidative stress and inflammation indices (C-reactive protein [CRP]) were measured and analyzed. A BA equation was proposed based on selected parameters, with terminal telomere restriction fragment (TRF) and CA as the two principal components. The selected aging markers included mitral annulus peak E anterior wall (MVEA), intima-media thickness (IMT), cystatin C (CYSC), D-dimer (DD), and digital symbol test (DST). The BA equation was: BA = −2.281TRF + 26.321CYSC + 0.025DD − 104.419MVEA + 34.863IMT − 0.265DST + 0.305CA + 26.346. To conclude, telomere length and CA as double benchmarks may be a new method to build a BA.
- ↑ 23.0 23.1 23.2 23.3 23.4 23.5 23.6 23.7 Zhang W et al.: Model Construction for Biological Age Based on a Cross-Sectional Study of a Healthy Chinese Han population. J Nutr Health Aging 2017. (PMID 29188884) [PubMed] [DOI] OBJECTIVES: Biological age (BA) has been proposed to evaluate the aging status in an objective way instead of chronological age (CA). The purpose of our study is to construct a more precise formula of BA in the cross-sectional study based on a largest-ever sample of our studies. This formula aims at better evaluation of body function and exploring the disciplines of aging in different genders and age stages. METHODS: A total of 1,373 healthy Chinese Han (age range, 19-93 years) were recruited from five cities in China, including 581 males and 792 females. Physical examination, blood routine, blood chemistry, and other lab tests were performed to obtain a total of 74 clinical variables. Then, the principal component analysis (PCA) was used to select variables and estimate BA. The BA formula was further validated in a population with some diseases (n=266), including cardiovascular diseases, type 2 diabetes, kidney diseases, pulmonary diseases, cancer and disorders in nervous system. RESULTS: The BA formula was constructed as follows: BA = 0.358 (pulse pressure) + 0.258 (trail making test) - 11.552 (mitral valve E/A peak) + 26.383 (minimum intima-media thickness) + 31.965 (Cystatin C) + 0.163 (CA) - 3.902. In validation of the formula, BAs of patients were older than those of healthy persons. The BA accelerates faster in the middle-aged population than in the elderly population (>75 years old). CONCLUSION: This BA formula can reflect health condition changes of aging better than CA in a Chinese Han population.
- ↑ 24.00 24.01 24.02 24.03 24.04 24.05 24.06 24.07 24.08 24.09 24.10 24.11 24.12 24.13 24.14 24.15 24.16 24.17 Nakamura E et al.: Biological age versus physical fitness age in women. Eur J Appl Physiol Occup Physiol 1990. (PMID 2282902) [PubMed] [DOI] The purpose of this study was to determine whether adult women who are in a state of high physical fitness are in a good state biologically, in terms of biological and physical fitness ages as estimated by statistical means. The subjects were 65 healthy Japanese women (aged 20-64 years). Biological and physical fitness ages were estimated from the data for 18 physiological function tests and 5 physical fitness tests, respectively, by a principal component model. The correlation coefficient between biological and physical fitness ages was 0.70 (P less than 0.01), which was generally regarded as a high correlation. Therefore, those who were in a state of high physical fitness were considered to be in good biological condition. This result is in good agreement with the results (r = 0.72) from adult men, on whom we reported previously. A statistical analysis to ascertain the relative importance of each contributory variable associated with the variance in biological age suggested that routine clinical evaluation of blood pressure and lipid metabolism might play an important role in determining not only the presence and severity of vascular disease but also the rate of biological aging in women.
- ↑ 25.0 25.1 25.2 25.3 25.4 25.5 25.6 25.7 25.8 25.9 Nakamura E & Miyao K: A method for identifying biomarkers of aging and constructing an index of biological age in humans. J Gerontol A Biol Sci Med Sci 2007. (PMID 17921421) [PubMed] [DOI] This study was conducted to identify biomarkers of aging and to construct an index of biological age in humans. Healthy adult men (n = 86) who had received an annual health examination from 1992 through 1998 were studied. From 29 physiological variables, five variables (forced expiratory volume in 1 second, systolic blood pressure, hematocrit, albumin, blood urea nitrogen) were selected as candidate biomarkers of aging. Five candidate biomarkers expressed substantial covariance along one principal component. The first principal component obtained from a principal component analysis was used to calculate biological age scores (BAS). Individual BAS showed high longitudinal stability of age-related changes. Age-related changes of BAS are characterized by three components: age, peak functional capacity, and aging rate. A logistic regression analysis suggested that aging rate was influenced by environmental factors, but peak functional capacity was almost independent of environmental factors.
- ↑ 26.00 26.01 26.02 26.03 26.04 26.05 26.06 26.07 26.08 26.09 26.10 26.11 26.12 26.13 26.14 26.15 26.16 26.17 26.18 26.19 26.20 26.21 Park J et al.: Developing a biological age assessment equation using principal component analysis and clinical biomarkers of aging in Korean men. Arch Gerontol Geriatr 2009. (PMID 18597867) [PubMed] [DOI] The purpose of the present study is to find clinically useful candidate biomarkers of aging, and using these to develop an equation measuring biological age (BA) in Korean men, then to validate the clinical usefulness of it. Among 4288 men who received medical health examinations, we selected 1588 men who met the normality criteria of each variable. We assumed that chronological ages (CA) of healthy persons represent the BA of them. Variables showing significant correlations with CA were selected. Redundant variables were excluded. We selected 11 variables: VO(2)max, percent body fat (%BF), waist circumference (WC), forced expiratory volume in 1 s (FEV1), systolic blood pressure (SBP), low density cholesterol (LDLCH), blood urea nitrogen (BUN), serum albumin (SA), erythrocyte sedimentation rate(ESR) hearing threshold (HT), and glycosylated hemoglobin (HBA1C). These 11 variables were then submitted into principal component analysis (PCA) and standardized BA scores were obtained. Using them and T-scale idea, the following equation to assess BA was developed: BA=-28.7+0.83(%BF)+0.48(WC)+0.13(SBP)-0.27(VO(2)max)+0.19(HT)-3.1(FEV1)+0.32(BUN)+0.06(LDLCH)-3.0(SA)+0.34(ESR)+4.6(HBA1C). We compared the BA of 3122 men by their fasting glucose and age level. The BA of the higher glucose level group was significantly higher than that of others at all CA levels. The selected 11 biomarkers encompassed known clinically important factors of adult diseases and functional disabilities. This BA assessment equation can be used in the general Korean male population and it proved to be clinically useful.
- ↑ 27.0 27.1 27.2 27.3 27.4 27.5 27.6 27.7 27.8 27.9 Ueno LM et al.: Biomarkers of aging in women and the rate of longitudinal changes. J Physiol Anthropol Appl Human Sci 2003. (PMID 12672981) [PubMed] [DOI] The purposes of this study were (1) to estimate biological age score (BAS) in Japanese healthy women based on the 4-7 years longitudinal data for physiological, hematological and biochemical examinations and (2) to examine the rate of aging changes in adult women based on the estimated BAS. The samples consisted of cross-sectional (n=981) and longitudinal (n=110) groups. Out of 31 variables examined, five variables (forced expiratory volume in 1.0 s, systolic blood pressure, mean corpuscular hemoglobin, glucose, albumin/globulin ratio) that met the following criteria: 1) significant cross-sectional correlation with age; 2) significant longitudinal change in the same direction as the cross-sectional correlation; and (3) assessment of redundancy, were selected as candidate biomarkers of aging. This variable set was then submitted into a principal component analysis, and the first principal component obtained from this analysis was used as an equation for assessing one's BAS. Individual BAS showed a high longitudinal stability of age-related changes, suggesting high predictive validity of our newly developed aging measurement equation. However, changes in the aging rate based on the estimated BAS were not constant. The mean slopes of the regression lines of BAS for the three age groups (age<45, 45</=age<65 yrs, 65</=age) were 0.095, 0.065, 0.138, respectively. One-way analysis of variance detected a significant difference (F=5.14, p<0.01) among the three age groups. These results suggest that the rate of aging in adult women is relatively slower until 65 years of age, but after 65, the rate of aging shows a rapid increase. We concluded that the longitudinal method used for selection of variables to compute the BAS was useful and theoretically valid compared to those obtained from cross-sectional data analysis.
- ↑ 28.0 28.1 28.2 28.3 28.4 28.5 28.6 28.7 28.8 28.9 Nakamura E & Miyao K: Sex differences in human biological aging. J Gerontol A Biol Sci Med Sci 2008. (PMID 18840798) [PubMed] [DOI] This study aims to clarify sex differences in human biological aging and to explore the gender gaps in health and longevity. Eighty-six men and 93 women who received a 2-day routine health checkup for 6-7 years beginning in 1992 at the Kyoto Red Cross Hospital were selected. Five candidate biomarkers of aging (forced expiratory volume in 1.0 second per square of height [FEV(1)/Ht(2)], systolic blood pressure [SBP], red blood cells [RBC], albumin [ALBU], and blood urea nitrogen [BUN]) were selected from 29 physiological variables. Individual biological ages (BAS) were estimated from these five biomarkers by a principal component model. From the investigation of the longitudinal changes of individual BAS, it was suggested that (i) beyond 65 years, the rate of aging showed a rapid increase, and (ii) women had relatively lower functional capabilities compared with men, but the rate of aging was slower than that of men, suggesting that these differences might present both disadvantages and advantages for women with regard to health and longevity.
- ↑ 29.00 29.01 29.02 29.03 29.04 29.05 29.06 29.07 29.08 29.09 29.10 29.11 29.12 29.13 29.14 Nakamura E et al.: Effects of habitual physical exercise on physiological age in men aged 20-85 years as estimated using principal component analysis. Eur J Appl Physiol Occup Physiol 1996. (PMID 8803500) [PubMed] [DOI] A population of 221 healthy adult men (aged 20-85 years) was studied to determine whether those who exercised regularly were in good biological condition, and also whether those who were in a state of high physical fitness were in a good state biologically, in terms of physiological age (PA) and physical fitness age (FA) as estimated by principal component analysis. A group of 17 physiological function tests and 5 physical fitness tests were employed to estimate PA and FA, respectively. The results of this study indicated that those who maintained high physical fitness at all age decade groups from 20 to 79 years had a trend towards maintaining a relatively lower PA (physiologically younger). Mean PA and FA of the trained group were younger by 4.7 and 7.3 years, respectively than those of the untrained group. In addition, the slope of regression line of PA on chronological age was more gentle in the trained group than that in the untrained group. These results would suggest that those who are in a state of high physical fitness maintain a relatively good physiological condition, and that regular physical exercise may delay physiological changes normally seen with aging, and consequently may increase the life span.
- ↑ 30.0 30.1 30.2 30.3 30.4 Borkan GA & Norris AH: Assessment of biological age using a profile of physical parameters. J Gerontol 1980. (PMID 6967883) [PubMed] [DOI] The present study describes a new approach to the assessment of biological age in adults using a profile of physical parameters. The investigation was based on data from 1086 adult male participants in the aging study of the Gerontology Research Ctr., Baltimore, MD. For each of 24 age-related variables, data were transformed into biological age scores reflecting a man's status relative to his chronological age peers. Analysis of the mean biological age profiles of men who were estimated by physicians as looking older than their age showed them to be biologically older on the profile parameters as well. Comparison of age-corrected scores of 166 men who have died with those of survivors reveals the deceased group to have been biologically older than the survivors at the time they were measured. These results suggest the value of this technique in investigating interindividual variation in the aging process.
- ↑ 31.00 31.01 31.02 31.03 31.04 31.05 31.06 31.07 31.08 31.09 31.10 31.11 Zhang WG et al.: Construction of an integral formula of biological age for a healthy Chinese population using principle component analysis. J Nutr Health Aging 2014. (PMID 24522464) [PubMed] [DOI] BACKGROUND: Whereas chronological age (CA) cannot distinguish functional differences among individuals of the same age, the biological age (BA) may be used to reflect the functional state of the body. The purpose of this study was to construct an integral formula of the BA, by using principle component analysis (PCA). METHODS: The vital organ function of 505 healthy individuals of Han origin (age 35-91 years) was examined. A total of 114 indicators of cardiovascular, pulmonary, and brain functions, and clinical, inflammatory, genetic, psychological, and life habit factors were assessed as candidate indicators of aging. Candidate indicators were submitted with CA to correlation and redundancy analyses. The PCA method was used to build an integral formula of the BA for the population. RESULTS: Seven biomarkers were selected in accordance with a certain load standard. These biomarkers included the trail making test (TMT), pulse pressure (PP), mitral valve annulus ventricular septum of the peak velocity of early filling (MVES), minimum carotid artery intimal-medial thickness (IMTmin), maximum internal diameter of the carotid artery (Dmax), maximal midexpiratory flow rate 75/25 (MMEF75/25), and Cystatin C (CysC). The formula for the BA was: BA = 0.0685 (TMT) + 0.267 (PP) - 1.375 (MVES) + 22.443 (IMTmin) + 2.962 (Dmax) - 2.332 (MMEF75/25) + 16.104 (CysC) + 0.137 (CA) + 0.492. CONCLUSION: Several genetic and lifestyle indicators were considered as candidate markers of aging. However, ultimately, only markers reflecting the function of the vital organs were included in the BA formula. This study represents a useful attempt to employ multiple indicators to build a comprehensive BA evaluation formula of aging populations.
- ↑ 32.00 32.01 32.02 32.03 32.04 32.05 32.06 32.07 32.08 32.09 32.10 32.11 32.12 Jee H et al.: Development and application of biological age prediction models with physical fitness and physiological components in Korean adults. Gerontology 2012. (PMID 22433233) [PubMed] [DOI] BACKGROUND: Several biological age (BA) prediction models have been suggested with a variety of biomarkers. Valid models should be able to measure BA in a relatively short time period and predict subsequent physiological capability. Physiological and physical fitness variables have been shown to be distinctive markers for predicting BA and morbidity. The practical and noninvasive nature of such variables makes them useful as clinical assessment tools in estimating BA for in-depth diagnosis and corresponding intervention. OBJECTIVE: To identify, develop and evaluate biomarkers and BA prediction models and validate their clinical usefulness for the practical diagnosis of functional aging. METHODS: Fourteen variables were measured in 3,112 male and 1,233 female participants aged 30 and older between the years 2004 and 2007. Through a series of parsimonious stepwise elimination processes, two sets of 8 gender-specific variables were selected as candidate biomarkers for 1,604 men and 760 women. Principal component analysis, linear regression analysis and adjustment methods were further applied to obtain two sets of true BA (TBA) prediction models. The TBA models were examined for validity by comparing TBA to the corresponding chronological age (CA) with clinical risk factors. RESULTS: TBA prediction models with r(2) values of 0.638 and 0.672 were developed, each unique to men and women, respectively. The overall mean TBA and CA of the participants were 53.9 and 51.8 years, respectively, with a marginal difference of -2.1 and -1.3 years. The regression slopes or rates of TBA as a function of CA were 1.00 and 1.28 for men and women with r values of 0.799 and 0.820 (p < 0.001), respectively. In comparing TBA to CA rates between healthy and clinical risk groups, both sarcopenic and obese groups showed significant increases in TBA. CONCLUSIONS: The selected biomarkers encompass various complex physiopathological factors related to intrinsic and extrinsic physiological and functional aging. The BA prediction models based on the selected biomarkers could be practical in assessing BA for Korean adults.
- ↑ 33.0 33.1 33.2 33.3 33.4 33.5 33.6 33.7 33.8 33.9 Hochschild R: Improving the precision of biological age determinations. Part 2: Automatic human tests, age norms and variability. Exp Gerontol 1989. (PMID 2583248) [PubMed] [DOI] In order to eliminate variability due to test operators, procedures for measuring 12 physiological functions that are candidate biomarkers of aging have been automated. Data was collected from a norm group of 2462 male and female office workers using an instrument which requires no test operators, administers all 12 tests in about 45 min. per subject, computes biological age, prints out results, and stores data on floppy disks for transfer to other computers for analysis. This report a) describes the instrumentation and test procedures, b) presents normal age/sex standards for each of the 12 biomarkers, c) reports the variance of the data for each biomarker by sex, d) lists sources of biomarker variance, e) discusses criteria for biomarker selection and f) examines implications for information loss when biomarker data is combined to calculate biological age. After eliminating chronological age as a variable, the standard deviations of the frequency distributions of predicted age for individual biomarkers were found to vary from .226 to 1.075, a range of more than 4 to 1. Procedures are discussed for improving the ratio of useful-to-useless variance in calculating biological age.
- ↑ 34.0 34.1 Zhang WG et al.: Peripheral Blood Leukocyte Telomere Length Is Associated with Age but Not Renal Function: A Cross-Sectional Follow-Up Study. J Nutr Health Aging 2018. (PMID 29380856) [PubMed] [DOI] OBJECTIVES: We aimed to evaluate the relationship between baseline renal function and changes in telomere length in Han Chinese. METHODS: The telomere restriction fragment (TRF) length of leukocytes in the peripheral blood was measured in healthy volunteers recruited in 2014. The estimated glomerular filtration rate (eGFR) was calculated based on serum creatinine (Scr) and serum cystatin C (CysC)-eGFRcys and eGFRScr-cys through the Cockcroft-Gault formula (eGFRC-G) or the Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI / eGFRCKD-EPI) equation. The correlation between telomere length changes over time and renal function was analyzed. RESULTS: Leukocyte TRF lengths were negatively correlated to age (r = -0.393, p < 0.001) and serum CysC (r = -0.180, p < 0.01), while positively associated with eGFRCKD-EPI, eGFRC-G, eGFRcys, and eGFRScr-cys (r = 0.182, 0.122, 0.290, and 0.254 respectively, p < 0.01). The 3-year change of telomere length was 46 bp/years. When adjusted for age, the associations between telomere length changes and baseline, subsequent TRF lengths, and serum CysC were no longer present. No association was observed between TRF length changes and renal function. CONCLUSION: The rate of telomere length changes was affected by age and baseline telomere length. The telomere length changes might be important markers for aging.
- ↑ 35.0 35.1 35.2 35.3 35.4 35.5 35.6 35.7 Voitenko VP & Tokar AV: The assessment of biological age and sex differences of human aging. Exp Aging Res 1983. (PMID 6667707) [PubMed] [DOI] Biological age can be assessed by means of clinical parameters. Some parameters are more suitable than others; criteria for a rational selection of such parameters are discussed in detail. The main tool used in this essay is multiple linear regression. The data reveal a characteristic sex difference in human and, presumably, mammalian aging.
- ↑ 36.00 36.01 36.02 36.03 36.04 36.05 36.06 36.07 36.08 36.09 36.10 36.11 36.12 36.13 36.14 36.15 Bae CY et al.: Development of models for predicting biological age (BA) with physical, biochemical, and hormonal parameters. Arch Gerontol Geriatr 2008. (PMID 17889950) [PubMed] [DOI] Individual differences are the hallmark of aging. Chronological age (CHA) is known that fails to provide an accurate indicator of the aging but biological age (BA) estimates the functional status of an individual in reference to his or her chronological peers on the basis of how well he or she functions in comparison with others of the same CHA. Therefore, we developed models for predicting BA that can be applicable in clinical practice settings. This was a community-based cross-sectional study. Subjects were recruited from the health promotion center in Korea from 2001 to 2005. Among these, data obtained from the 3575 participants (1302 men and 2273 women) was used for clinical evaluation and statistical analysis. For our test battery we selected 25 parameters among the routine tests. For males, the best models were developed using 15, 7, 5, and 4 of the 25 chosen parameters for total, physical, biochemical and hormonal characteristics, respectively (R(2)=0.62, 0.38, 0.33, and 0.36, respectively). Similar to males, for the females, 14, 6, 8, and 3 parameters were developed as the models (R(2)=0.66, 0.40, 0.42, and 0.37, respectively). Our BA prediction models may be used as supplementary tools adding knowledge in the evaluation of aging status.
- ↑ 37.00 37.01 37.02 37.03 37.04 37.05 37.06 37.07 37.08 37.09 37.10 37.11 37.12 37.13 37.14 37.15 37.16 37.17 37.18 37.19 37.20 37.21 37.22 37.23 37.24 37.25 37.26 37.27 37.28 37.29 37.30 37.31 37.32 Bae CY et al.: Models for estimating the biological age of five organs using clinical biomarkers that are commonly measured in clinical practice settings. Maturitas 2013. (PMID 23642770) [PubMed] [DOI] OBJECTIVES: To date, no worldwide studies have been conducted to estimate the biological age of five organs using clinical biomarkers that are associated with the aging status. Therefore, we conducted this study to develop the models for estimating the biological age of five organs (heart, lung, liver, pancreas, and kidney) using clinical biomarkers which are commonly measured in clinical practice. DESIGN: A cross sectional study. METHODS: Subjects were recruited from the routine health check-up centers in Korea from 2004 through 2010. Data obtained from 121,189 subjects (66,168 men and 55,021 women) were used for clinical evaluation and statistical analysis. We examined the relations between clinical biomarkers associated with five organs and the chronological age and proposed a model for estimating the biological age of five organs. RESULTS: In the models for predicting the biological ages of the heart, lung, liver, pancreas and kidney in men, 12, 2, 8, 3, and 5 parameters were respectively included (R(2)=0.652, 0.427, 0.107, 0.245, and 0.651). In contrast to men, 10, 2, 8, 3, and 5 parameters in women were respectively included (R(2)=0.780, 0.435, 0.140, 0.384, and 0.501). CONCLUSION: We first proposed the models for predicting the biological age of five organs in the current study. We developed those using clinical parameters that can be easily obtained in clinical practice settings. Our biological age prediction models may be used as supplementary tools to assess the aging status of five organs in clinical practice settings.
- ↑ 38.00 38.01 38.02 38.03 38.04 38.05 38.06 38.07 38.08 38.09 38.10 38.11 38.12 38.13 38.14 38.15 38.16 Jee H: Selection of a set of biomarkers and comparisons of biological age estimation models for Korean men. J Exerc Rehabil 2019. (PMID 30899733) [PubMed] [DOI] [Full text] Biological age (BA) represents the rate of the senescence with a set of biomarkers. The BA prediction models have not been compared to obtain an optimal BA prediction model with BA biomarkers for Korean men. The study aims to obtain a set of BA biomarkers and compare three of the reported statistical approaches for an optimal BA prediction model. The Korea National Health and Nutrition Examination Surveys data of 2009 to 2011 were used to select six BA biomarkers from 940 healthy subjects aged between 30 to 80 years. The multiple linear regression (MLR), principal component analysis (PCA), and Klemera and Doubal methods (KDM) were used to obtain three BA prediction models. Correlation coefficients (r) with 95% confidence intervals (CI) and regression slopes were assessed. One of the Euro Quality of Life-5 Dimensions, mobility, was compared for feasibility test of each BA models. KDM showed greatest correlation (r=0.88 [P<0.05]) with smallest 95% CI and regression slope (1.00). PCA also showed strong correlation (r=0.79 [P<0.05]) with small 95% CI and regression slope (0.94). MLR (r=0.68 [P<0.05]) showed over and underestimated BA results at the end of the age spectrum. Estimations of BA were most reliable with KDM. The PCA and MLR approaches were comparatively simple to devise for Korean men.
- ↑ 39.0 39.1 39.2 39.3 39.4 39.5 39.6 39.7 39.8 Nakamura E & Miyao K: Further evaluation of the basic nature of the human biological aging process based on a factor analysis of age-related physiological variables. J Gerontol A Biol Sci Med Sci 2003. (PMID 12634284) [PubMed] [DOI] This study aimed to reexamine whether there exists a primary aging process that controls the rate of aging in a number of different functions. Eighty-six adult males who successively received a 2-day routine health checkup test for 7 years from 1992 to 1998 at the Kyoto Red Cross Hospital were selected as subjects. Nine candidate biomarkers of aging were selected from the 25 physiological variables based on the investigation of age-related changes. A principal factor analysis was applied to the partial correlation matrix for 9 selected biomarkers calculated by controlling for age. Furthermore, a confirmatory factor analysis in testing first- and second-order factor models was applied to the covariance matrix for 9 biomarkers. The results of these factor analyses revealed that there existed one general factor and three system-specific factors. Therefore, biological age changes can be viewed as a time-dependent complex integration of the primary and secondary aging processes.
- ↑ 40.0 40.1 40.2 40.3 40.4 40.5 40.6 40.7 40.8 40.9 Belsky DW et al.: Quantification of biological aging in young adults. Proc Natl Acad Sci U S A 2015. (PMID 26150497) [PubMed] [DOI] [Full text] Antiaging therapies show promise in model organism research. Translation to humans is needed to address the challenges of an aging global population. Interventions to slow human aging will need to be applied to still-young individuals. However, most human aging research examines older adults, many with chronic disease. As a result, little is known about aging in young humans. We studied aging in 954 young humans, the Dunedin Study birth cohort, tracking multiple biomarkers across three time points spanning their third and fourth decades of life. We developed and validated two methods by which aging can be measured in young adults, one cross-sectional and one longitudinal. Our longitudinal measure allows quantification of the pace of coordinated physiological deterioration across multiple organ systems (e.g., pulmonary, periodontal, cardiovascular, renal, hepatic, and immune function). We applied these methods to assess biological aging in young humans who had not yet developed age-related diseases. Young individuals of the same chronological age varied in their "biological aging" (declining integrity of multiple organ systems). Already, before midlife, individuals who were aging more rapidly were less physically able, showed cognitive decline and brain aging, self-reported worse health, and looked older. Measured biological aging in young adults can be used to identify causes of aging and evaluate rejuvenation therapies.
- ↑ 41.0 41.1 41.2 41.3 41.4 41.5 41.6 41.7 Brown PJ et al.: Biological Age, Not Chronological Age, Is Associated with Late-Life Depression. J Gerontol A Biol Sci Med Sci 2018. (PMID 28958059) [PubMed] [DOI] [Full text] BACKGROUND: The pathophysiology of late-life depression (LLD) is complex and heterogeneous, with age-related processes implicated in its pathogenesis. This study examined the cross-sectional and longitudinal association between depressive symptoms and a baseline multibiomarker algorithm of biological age (BA) that aggregates indicators of inflammatory, metabolic, cardiovascular, lung, liver, and kidney functioning. METHOD: Data were analyzed from 2,776 men and women from the prospective observational Health Aging and Body Composition Study, who had both evaluable chronological age (CA) and BA. Depressive symptoms were assessed using the Center for Epidemiologic Studies Depression (CES-D) scale. RESULTS: A covariate-adjusted regression model showed that BA (B = 0.03, p = .0471) but not CA (B = -0.01, p = .7185) is associated with baseline CES-D scores. The mean baseline BA for individuals with a CES-D ≥ 10 was 1.28 years greater than in those with a CES-D < 10. Comparatively, there is only a 0.05-year difference in mean CA between the two depression groups. A covariate-adjusted longitudinal model found that baseline BA predicts CES-D score at follow-up (B = 0.04, p = .0058), whereas CA does not (B = 0.03, p = .4125). Additionally, an older BA significantly predicted a CES-D ≥ 10 (B = 0.02, p = .032) over a 10-year period. CONCLUSIONS: A multibiomarker index of an older adult's BA outperformed their CA in predicting subsequent increased and clinically significant depressive symptoms. This result supports the evolving view of LLD as a brain disorder resulting from deleterious age-associated changes across numerous physiological systems.
- ↑ 42.0 42.1 42.2 42.3 42.4 42.5 42.6 Murabito JM et al.: Measures of Biologic Age in a Community Sample Predict Mortality and Age-Related Disease: The Framingham Offspring Study. J Gerontol A Biol Sci Med Sci 2018. (PMID 28977464) [PubMed] [DOI] [Full text] BACKGROUND: We tested the association of biologic age (BA) measures constructed from different types of biomarkers with mortality and disease in a community-based sample. METHODS: In Framingham Offspring participants at Exams 7 (1998-2001, mean age 62 ± 10) and 8 (2005-2008, mean age 67 ± 9), we used the Klemera-Doubal method to estimate clinical BA and inflammatory BA and computed the difference (∆age) between BA and CA. Clinical ∆age was computed at Exam 2 (1979-1983, mean age 45 ± 10). At Exam 8, we computed measures of intrinsic and extrinsic epigenetic age. Participants were followed through 2014 for outcomes. Cox proportional hazards models tested the association of each BA estimate with each outcome adjusting for covariates. RESULTS: Sample sizes ranged from 2532 to 3417 participants. In multivariable models, each 1-year increase in clinical ∆age at Exam 2 (hazard ratio [HR] = 1.04-1.06, p < 2 × 10-16) and clinical ∆age and inflammatory ∆age at Exam 7 significantly increased the hazards of mortality and incident cardiovascular disease (HR = 1.01-1.05, p < 2 × 10-7), whereas inflammatory ∆age increased the hazards of cancer (HR = 1.01, p < .05). At Exam 8, increased clinical ∆age, inflammatory ∆age, and extrinsic epigenetic age all significantly increased the hazard of mortality (HR = 1.03-1.05, all p < .05); clinical ∆age and inflammatory ∆age increased cardiovascular disease risk (HR = 1.04-1.05, all p < .01); and clinical ∆age increased cancer risk (HR = 1.03, p < .01) when all three BA measures were included in the model. Intrinsic epigenetic age was not significantly associated with any outcome. CONCLUSIONS: Our findings suggest BA measures may be complementary in predicting risk for mortality and age-related disease.
- ↑ 43.00 43.01 43.02 43.03 43.04 43.05 43.06 43.07 43.08 43.09 43.10 43.11 Hastings WJ et al.: Comparability of biological aging measures in the National Health and Nutrition Examination Study, 1999-2002. Psychoneuroendocrinology 2019. (PMID 30999227) [PubMed] [DOI] [Full text] BACKGROUND: Biological processes of aging are thought to be modifiable causes of many different chronic diseases. Measures of biological aging could provide sensitive endpoints for studies of risk factors hypothesized to shorten healthy lifespan and/or interventions that extend it. But uncertainty remains about how to measure biological aging and if proposed measures assess the same thing. METHOD: We tested four proposed measures of biological aging that could be quantified with available data from the National Health and Nutrition Examination Survey (NHANES), Klemera-Doubal method (KDM) Biological Age, homeostatic dysregulation, Levine Method (LM) Biological Age, and leukocyte telomere length. RESULTS: We analyzed data collected during 1999-2002, when all four biological aging meausres could be taken. Participants' KDM biological ages, homeostatic dysregulation levels, LM biological ages, and telomere length were all correlated with their chronological ages. KDM Biological Age, homeostatic dysregulation, and LM Biological Age were all correlated with one another, but these measures were uncorrelated with telomere length. Participants' with more advanced biological aging performed worse on tests of physical, cognitive, and perceptual functioning and reported more limitations to their daily activities and more pain, and rated themselves as being in worse health. In parallel, participants with risk factors for shorter healthy lifespan exhibited more advanced biological aging. In both sets of analyses, effect-sizes tended to be larger for KDM Biological Age, homeostatic dysregulation, and LM Biological Age as compared to telomere length. DISCUSSION: The cellular-level aging biomarker telomere length may measure different aspects of the aging process as compared to the patient-level physiological composite measures KDM Biological Age, homeostatic dysregulation, and LM Biological Age. Studies aiming to test if risk factors accelerate aging or if interventions may slow aging should not treat proposed measures of aging as interchangeable.
- ↑ 44.00 44.01 44.02 44.03 44.04 44.05 44.06 44.07 44.08 44.09 44.10 Gaydosh L et al.: Testing Proposed Quantifications of Biological Aging in Taiwanese Older Adults. J Gerontol A Biol Sci Med Sci 2020. (PMID 31566204) [PubMed] [DOI] [Full text] Quantification of biological aging is of interest in gerontology as a means to surveil aging rates in the population and to evaluate the effects of interventions to increase healthy life span. Analysis of proposed methods to quantify biological aging has focused on samples of midlife or mixed-age adults in the West. Research is needed to test whether quantifications of biological aging can differentiate aging rates among older adults and if quantifications of biological aging developed in Western samples can differentiate aging rates in non-Western populations. We conducted analysis of Klemera-Doubal method (KDM) Biological Age and homeostatic dysregulation measures of biological aging developed in the U.S. NHANES and tested in a sample of older Taiwanese adults in the Social Environment and Biomarkers of Aging Study. We conducted analysis of physical and cognitive function and mortality, comparing quantifications of biological aging to a biomarker index based on norms within our analysis sample and to participants' ratings of their own health. Results showed that quantifications of biological aging (a) predicted differences in physical and cognitive function and in mortality risk among Taiwanese older adults and (b) performed as well as a traditional biomarker index and participant self-rated health for prediction of these outcomes.
- ↑ 45.00 45.01 45.02 45.03 45.04 45.05 45.06 45.07 45.08 45.09 45.10 45.11 Liu Z: Development and Validation of 2 Composite Aging Measures Using Routine Clinical Biomarkers in the Chinese Population: Analyses From 2 Prospective Cohort Studies. J Gerontol A Biol Sci Med Sci 2021. (PMID 32946548) [PubMed] [DOI] [Full text] BACKGROUND: This study aimed to: (i) develop 2 composite aging measures in the Chinese population using 2 recent advanced algorithms (the Klemera and Doubal method and Mahalanobis distance); and (ii) validate the 2 measures by examining their associations with mortality and disease counts. METHODS: Based on data from the China Nutrition and Health Survey (CHNS) 2009 wave (N = 8119, aged 20-79 years, 53.5% women), a nationwide prospective cohort study of the Chinese population, we developed Klemera and Doubal method-biological age (KDM-BA) and physiological dysregulation (PD, derived from Mahalanobis distance) using 12 biomarkers. For the validation analysis, we used Cox proportional hazard regression models (for mortality) and linear, Poisson, and logistic regression models (for disease counts) to examine the associations. We replicated the validation analysis in the China Health and Retirement Longitudinal Study (CHARLS, N = 9304, aged 45-99 years, 53.4% women). RESULTS: Both aging measures were predictive of mortality after accounting for age and gender (KDM-BA, per 1-year, hazard ratio [HR] = 1.14, 95% confidence interval [CI] = 1.08, 1.19; PD, per 1-SD, HR = 1.50, 95% CI = 1.33, 1.69). With few exceptions, these mortality predictions were robust across stratifications by age, gender, education, and health behaviors. The 2 aging measures were associated with disease counts both cross-sectionally and longitudinally. These results were generally replicable in CHARLS although 4 biomarkers were not available. CONCLUSIONS: We successfully developed and validated 2 composite aging measures-KDM-BA and PD, which have great potentials for applications in early identifications and preventions of aging and aging-related diseases in China.
- ↑ 46.0 46.1 46.2 46.3 46.4 46.5 46.6 Kuo CL et al.: Genetic associations for two biological age measures point to distinct aging phenotypes. Aging Cell 2021. (PMID 34038024) [PubMed] [DOI] [Full text] Biological age measures outperform chronological age in predicting various aging outcomes, yet little is known regarding genetic predisposition. We performed genome-wide association scans of two age-adjusted biological age measures (PhenoAgeAcceleration and BioAgeAcceleration), estimated from clinical biochemistry markers (Levine et al., 2018; Levine, 2013) in European-descent participants from UK Biobank. The strongest signals were found in the APOE gene, tagged by the two major protein-coding SNPs, PhenoAgeAccel-rs429358 (APOE e4 determinant) (p = 1.50 × 10-72 ); BioAgeAccel-rs7412 (APOE e2 determinant) (p = 3.16 × 10-60 ). Interestingly, we observed inverse APOE e2 and e4 associations and unique pathway enrichments when comparing the two biological age measures. Genes associated with BioAgeAccel were enriched in lipid related pathways, while genes associated with PhenoAgeAccel showed enrichment for immune system, cell function, and carbohydrate homeostasis pathways, suggesting the two measures capture different aging domains. Our study reaffirms that aging patterns are heterogeneous across individuals, and the manner in which a person ages may be partly attributed to genetic predisposition.
- ↑ 47.00 47.01 47.02 47.03 47.04 47.05 47.06 47.07 47.08 47.09 47.10 47.11 47.12 47.13 47.14 47.15 47.16 47.17 47.18 47.19 47.20 47.21 47.22 47.23 47.24 47.25 47.26 47.27 47.28 47.29 Zhong X et al.: Estimating Biological Age in the Singapore Longitudinal Aging Study. J Gerontol A Biol Sci Med Sci 2020. (PMID 31179487) [PubMed] [DOI] BACKGROUND: Biological age (BA) is a more accurate measure of the rate of human aging than chronological age (CA). However, there is limited consensus regarding measures of BA in life span and healthspan. METHODS: This study investigated measurement sets of 68 physiological biomarkers using data from 2,844 Chinese Singaporeans in two age subgroups (55-70 and 71-94 years) in the Singapore Longitudinal Aging Study (SLAS-2) with 8-year follow-up frailty and mortality data. We computed BA estimate using three commonly used algorithms: Principal Component Analysis (PCA), Multiple Linear Regression (MLR), and Klemera and Doubal (KD) method, and additionally, explored the use of machine learning methods for prediction of mortality and frailty. The most optimal algorithmic estimate of BA compared to CA was evaluated for their associations with risk factors and health outcome. RESULTS: Stepwise selection procedures resulted in the final selection of 8 biomarkers in males and 10 biomarkers in females. The highest-ranking biomarkers were estimated glomerular filtration rate for both genders, and the forced expiratory volume in 1 second in males and females. The BA estimates robustly predicted frailty and mortality and outperformed CA. The best performing KD measure of BA was notably predictive in the younger group (aged 55-70 years). BA estimates obtained using a machine learning train-test method were not more accurate than conventional BA estimates in predicting mortality and frailty in most situations. Biologically older people with the same CA as biologically younger individuals had higher prevalence of frailty and 8-year mortality, and worse health, behavioral, and functional characteristics. CONCLUSIONS: BA is better than CA for measuring life span (mortality) and healthspan (frailty). This measurement set of physiological markers of biological aging among Chinese robustly differentiate biologically old from younger individuals with the same CA.
- ↑ 48.0 48.1 48.2 48.3 48.4 48.5 48.6 48.7 48.8 48.9 Mitnitski A et al.: Heterogeneity of Human Aging and Its Assessment. J Gerontol A Biol Sci Med Sci 2017. (PMID 27216811) [PubMed] [DOI] [Full text] Understanding the heterogeneity in health of older adults is a compelling question in the biology of aging. We analyzed the performance of five measures of health heterogeneity, judging them by their ability to predict mortality. Using clinical and biomarker data on 1,013 participants of the Canadian Study of Health and Aging who were followed for up to 6 years, we calculated two indices of biological age using the Klemera and Doubal method, which controversially includes using chronological age as a "biomarker," and three frailty indices (FIs) that do not include chronological age: a standard clinical FI, an FI from standard laboratory blood tests and blood pressure, and their combination (FI-combined). Predictive validity was tested using Cox proportional hazards analysis and discriminative ability by the area under the receiver-operating characteristic curves. All five measures showed moderate performance that was improved by combining measures to evaluate larger numbers of items. The greatest addition in explanatory power came from the FI-combined that showed the best mortality prediction in an age-adjusted model. More extensive comparisons across different databases are required, but these results do not support including chronological age as a biomarker.
- ↑ 49.0 49.1 49.2 49.3 49.4 Kang YG et al.: Models for estimating the metabolic syndrome biological age as the new index for evaluation and management of metabolic syndrome. Clin Interv Aging 2017. (PMID 28203066) [PubMed] [DOI] [Full text] PURPOSE: This study aims to propose a metabolic syndrome (MS) biological age model, through which overall evaluation and management of the health status and aging state in MS can be done easily. Through this model, we hope to provide a novel evaluation and management health index that can be utilized in various health care fields. PATIENT AND METHODS: MS parameters from American Heart Association/National Heart, Lung, and Blood Institute guidelines in 2005 were used as biomarkers for the estimation of MS biological age. MS biological age model development was done by analyzing data of 263,828 participants and clinical application of the developed MS biological age was assessed by analyzing the data of 188,886 subjects. RESULTS: The principal component accounted for 36.1% in male and 38.9% in female of the total variance in the battery of five variables. The correlation coefficient between corrected biological age and chronological age in males and females were 0.711 and 0.737, respectively. Significant difference for mean MS biological age and chronological age between the three groups, normal, at risk and MS, was seen (P<0.001). CONCLUSION: For the comprehensive approach in MS management, MS biological age is expected to be additionally utilized as a novel evaluation and management index along with the traditional MS diagnosis.
- ↑ 50.0 50.1 50.2 50.3 Takeda H et al.: Evaluation of biological age and physical age by multiple regression analysis. Med Inform (Lond) 1982. (PMID 7162237) [PubMed] [DOI]
- ↑ 51.0 51.1 51.2 Dubina TL et al.: Biological age and its estimation. III. Introduction of a correction to the multiple regression model of biological age in cross-sectional and longitudinal studies. Exp Gerontol 1984. (PMID 6610563) [PubMed] [DOI] In order to eliminate systematic error inherent in assessment of an individual biological age (BA), a correction is suggested for the multiple regression model of BA. The larger the difference between an individual's chronological age and middle age of the sample, the greater the correction value. BA estimates of apparently healthy people of 60 to 100 years were assessed using measurements of three physiological indices: hand grip strength, short-time memory, and vibrotactile sensitivity. Introduction of the correction allowed comparison of BA estimates of the same individual obtained from repeated observations. Preliminary results show there are at least four types of the BA changes with advancing age.
- ↑ 52.0 52.1 52.2 52.3 52.4 52.5 52.6 52.7 52.8 52.9 Parker DC et al.: Association of Blood Chemistry Quantifications of Biological Aging With Disability and Mortality in Older Adults. J Gerontol A Biol Sci Med Sci 2020. (PMID 31693736) [PubMed] [DOI] [Full text] Quantification of biological aging has been proposed for population surveillance of age-related decline in system integrity and evaluation of geroprotective therapies. However, methods of quantifying biological aging have been little studied in geriatric populations. We analyzed three clinical-biomarker-algorithm methods to quantify biological aging. Klemera-Doubal method Biological Age and homeostatic dysregulation algorithms were parameterized from analysis of U.S. National Health and Nutrition Examination Surveys (NHANES) data (N = 36,207) based on published methods. Levine method Biological Age was adapted from published analysis of NHANES data. Algorithms were applied to biomarker data from the Duke Established Populations for Epidemiologic Studies of the Elderly (Duke-EPESE) cohort of older adults (N = 1,374, aged 71-102 years, 35% male, 52% African American). We tested associations of biological aging measures with participant reported Activities of daily living (ADL), instrumental activities of daily living (IADL) dependencies, and mortality. We evaluated the sensitivity of results to the demographic composition of reference samples and biomarker sets used to develop biological aging algorithms. African American and white Duke-EPESE participants with more advanced biological aging reported dependence in more ADLs and IADLs and were at increased risk of death over follow-up through 2017. Effect sizes were similar across algorithms, but were strongest for Levine method Biological Age (per-quintile increase in ADL incidence rate ratio = 1.25, 95% confidence interval [1.17-1.37], IADL incidence rate ratio = 1.23 [1.15-1.32], mortality hazard ratio = 1.12 [1.08-1.16]). Results were insensitive to demographic composition of reference samples, but modestly sensitive to the biomarker sets used to develop biological aging algorithms. Blood-chemistry-based quantifications of biological aging show promise for evaluating the effectiveness of interventions to extend healthy life span in older adults.
- ↑ Li Z et al.: Progress in biological age research. Front Public Health 2023. (PMID 37124811) [PubMed] [DOI] [Full text] Biological age (BA) is a common model to evaluate the function of aging individuals as it may provide a more accurate measure of the extent of human aging than chronological age (CA). Biological age is influenced by the used biomarkers and standards in selected aging biomarkers and the statistical method to construct BA. Traditional used BA estimation approaches include multiple linear regression (MLR), principal component analysis (PCA), Klemera and Doubal's method (KDM), and, in recent years, deep learning methods. This review summarizes the markers for each organ/system used to construct biological age and published literature using methods in BA research. Future research needs to explore the new aging markers and the standard in select markers and new methods in building BA models.
- ↑ Jylhävä J et al.: Biological Age Predictors. EBioMedicine 2017. (PMID 28396265) [PubMed] [DOI] [Full text] The search for reliable indicators of biological age, rather than chronological age, has been ongoing for over three decades, and until recently, largely without success. Advances in the fields of molecular biology have increased the variety of potential candidate biomarkers that may be considered as biological age predictors. In this review, we summarize current state-of-the-art findings considering six potential types of biological age predictors: epigenetic clocks, telomere length, transcriptomic predictors, proteomic predictors, metabolomics-based predictors, and composite biomarker predictors. Promising developments consider multiple combinations of these various types of predictors, which may shed light on the aging process and provide further understanding of what contributes to healthy aging. Thus far, the most promising, new biological age predictor is the epigenetic clock; however its true value as a biomarker of aging requires longitudinal confirmation.
- ↑ Erema VV et al.: Biological Age Predictors: The Status Quo and Future Trends. Int J Mol Sci 2022. (PMID 36499430) [PubMed] [DOI] [Full text] There is no single universal biomarker yet to estimate overall health status and longevity prospects. Moreover, a consensual approach to the very concept of aging and the means of its assessment are yet to be developed. Markers of aging could facilitate effective health control, more accurate life expectancy estimates, and improved health and quality of life. Clinicians routinely use several indicators that could be biomarkers of aging. Duly validated in a large cohort, models based on a combination of these markers could provide a highly accurate assessment of biological age and the pace of aging. Biological aging is a complex characteristic of chronological age (usually), health-to-age concordance, and medically estimated life expectancy. This study is a review of the most promising techniques that could soon be used in routine clinical practice. Two main selection criteria were applied: a sufficient sample size and reliability based on validation. The selected biological age calculators were grouped according to the type of biomarker used: (1) standard clinical and laboratory markers; (2) molecular markers; and (3) epigenetic markers. The most accurate were the calculators, which factored in a variety of biomarkers. Despite their demonstrated effectiveness, most of them require further improvement and cannot yet be considered for use in standard clinical practice. To illustrate their clinical application, we reviewed their use during the COVID-19 pandemic.
- ↑ Lohman T et al.: Predictors of Biological Age: The Implications for Wellness and Aging Research. Gerontol Geriatr Med 2021. (PMID 34595331) [PubMed] [DOI] [Full text] As healthspan and lifespan research breakthroughs have become more commonplace, the need for valid, practical markers of biological age is becoming increasingly paramount. The accessibility and affordability of biological age predictors that can reveal information about mortality and morbidity risk, as well as remaining years of life, has profound clinical and research implications. In this review, we examine 5 groups of aging biomarkers capable of providing accurate biological age estimations. The unique capabilities of these biomarkers have far reaching implications for the testing of both pharmaceutical and non-pharmaceutical interventions designed to slow or reverse biological aging. Additionally, the enhanced validity and availability of these tools may have increasingly relevant clinical value. The authors of this review explore those implications, with an emphasis on lifestyle modification research, and provide an overview of the current evidence regarding 5 biological age predictor categories: Telomere length, composite biomarkers, DNA methylation "epigenetic clocks," transcriptional predictors of biological age, and functional age predictors.
- ↑ Ashiqur Rahman S et al.: Deep learning for biological age estimation. Brief Bioinform 2021. (PMID 32363395) [PubMed] [DOI] [Full text] Modern machine learning techniques (such as deep learning) offer immense opportunities in the field of human biological aging research. Aging is a complex process, experienced by all living organisms. While traditional machine learning and data mining approaches are still popular in aging research, they typically need feature engineering or feature extraction for robust performance. Explicit feature engineering represents a major challenge, as it requires significant domain knowledge. The latest advances in deep learning provide a paradigm shift in eliciting meaningful knowledge from complex data without performing explicit feature engineering. In this article, we review the recent literature on applying deep learning in biological age estimation. We consider the current data modalities that have been used to study aging and the deep learning architectures that have been applied. We identify four broad classes of measures to quantify the performance of algorithms for biological age estimation and based on these evaluate the current approaches. The paper concludes with a brief discussion on possible future directions in biological aging research using deep learning. This study has significant potentials for improving our understanding of the health status of individuals, for instance, based on their physical activities, blood samples and body shapes. Thus, the results of the study could have implications in different health care settings, from palliative care to public health.